More than half of the publishers listed alongside IntechOpen (18 out of 30) are Social Science and Humanities publishers. IntechOpen is an exception to this as a leader in not only Open Access content but Open Access content across all scientific disciplines, including Physical Sciences, Engineering and Technology, Health Sciences, Life Science, and Social Sciences and Humanities.
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Our breakdown of titles published demonstrates this with 47% PET, 31% HS, 18% LS, and 4% SSH books published.
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“Even though ItechOpen has shown the potential of sci-tech books using an OA approach,” other publishers “have shown little interest in OA books.”
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Additionally, each book published by IntechOpen contains original content and research findings.
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We are honored to be among such prestigious publishers and we hope to continue to spearhead that growth in our quest to promote Open Access as a true pioneer in OA book publishing.
Simba Information has released its Open Access Book Publishing 2020 - 2024 report and has again identified IntechOpen as the world’s largest Open Access book publisher by title count.
\n\n
Simba Information is a leading provider for market intelligence and forecasts in the media and publishing industry. The report, published every year, provides an overview and financial outlook for the global professional e-book publishing market.
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IntechOpen, De Gruyter, and Frontiers are the largest OA book publishers by title count, with IntechOpen coming in at first place with 5,101 OA books published, a good 1,782 titles ahead of the nearest competitor.
\n\n
Since the first Open Access Book Publishing report published in 2016, IntechOpen has held the top stop each year.
\n\n\n\n
More than half of the publishers listed alongside IntechOpen (18 out of 30) are Social Science and Humanities publishers. IntechOpen is an exception to this as a leader in not only Open Access content but Open Access content across all scientific disciplines, including Physical Sciences, Engineering and Technology, Health Sciences, Life Science, and Social Sciences and Humanities.
\n\n
Our breakdown of titles published demonstrates this with 47% PET, 31% HS, 18% LS, and 4% SSH books published.
\n\n
“Even though ItechOpen has shown the potential of sci-tech books using an OA approach,” other publishers “have shown little interest in OA books.”
\n\n
Additionally, each book published by IntechOpen contains original content and research findings.
\n\n
We are honored to be among such prestigious publishers and we hope to continue to spearhead that growth in our quest to promote Open Access as a true pioneer in OA book publishing.
\n\n
\n\n
\n'}],latestNews:[{slug:"webinar-introduction-to-open-science-wednesday-18-may-1-pm-cest-20220518",title:"Webinar: Introduction to Open Science | Wednesday 18 May, 1 PM CEST"},{slug:"step-in-the-right-direction-intechopen-launches-a-portfolio-of-open-science-journals-20220414",title:"Step in the Right Direction: IntechOpen Launches a Portfolio of Open Science Journals"},{slug:"let-s-meet-at-london-book-fair-5-7-april-2022-olympia-london-20220321",title:"Let’s meet at London Book Fair, 5-7 April 2022, Olympia London"},{slug:"50-books-published-as-part-of-intechopen-and-knowledge-unlatched-ku-collaboration-20220316",title:"50 Books published as part of IntechOpen and Knowledge Unlatched (KU) Collaboration"},{slug:"intechopen-joins-the-united-nations-sustainable-development-goals-publishers-compact-20221702",title:"IntechOpen joins the United Nations Sustainable Development Goals Publishers Compact"},{slug:"intechopen-signs-exclusive-representation-agreement-with-lsr-libros-servicios-y-representaciones-s-a-de-c-v-20211123",title:"IntechOpen Signs Exclusive Representation Agreement with LSR Libros Servicios y Representaciones S.A. de C.V"},{slug:"intechopen-expands-partnership-with-research4life-20211110",title:"IntechOpen Expands Partnership with Research4Life"},{slug:"introducing-intechopen-book-series-a-new-publishing-format-for-oa-books-20210915",title:"Introducing IntechOpen Book Series - A New Publishing Format for OA Books"}]},book:{item:{type:"book",id:"7330",leadTitle:null,fullTitle:"Topics From EPR Research",title:"Topics From EPR Research",subtitle:null,reviewType:"peer-reviewed",abstract:"Electron paramagnetic resonance (EPR) spectroscopy has become one of the leading spectroscopic techniques. It targets materials containing unpaired electrons and possesses many applications. Since it was discovered more than 70 years ago, EPR spectroscopy is subjected to uninterrupted development and comprehensive studies. This book represents some of recent topics from EPR research.",isbn:"978-1-78985-300-1",printIsbn:"978-1-78985-299-8",pdfIsbn:"978-1-83962-013-3",doi:"10.5772/intechopen.75082",price:100,priceEur:109,priceUsd:129,slug:"topics-from-epr-research",numberOfPages:98,isOpenForSubmission:!1,isInWos:null,isInBkci:!1,hash:"b1997bf8b0968b84776a82777a3295c5",bookSignature:"Ahmed M. 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Maghraby graduated from Cairo University, Faculty of Science, Egypt, in 1995, and started his career as a scientist at the National Institute of Standards (NIS), Egypt. He received his MSc in 1999 and his Ph.D. from Cairo University in 2003 for his study on the calibration and characterization of organic material for use in radiation dosimetry using electron paramagnetic resonance (EPR). In 1999, Dr. Maghraby worked as a guest researcher at the National Institute of Standards and Technology (NIST) in Maryland, USA, and as a visiting scientist at Dartmouth College (EPR center of viable system) in New Hampshire, USA, in 2008. In 2006, he worked as a guest researcher for the Physikalisch-Technische Bundesanstalt (PTB), Germany’s national metrology institute. He has led and participated in several international research projects on radiation measurements. His research interest is ionizing radiation metrology, especially ionization chambers, EPR, and thermoluminescence dosimetry (TLD). He is a reviewer for several peer-reviewed journals and has supervised a number of master’s and Ph.D. theses, and was elected as the vice president of the National Committee of Physics (NPC) in Egypt.",institutionString:"National Institute of Standards",position:null,outsideEditionCount:0,totalCites:0,totalAuthoredChapters:"2",totalChapterViews:"0",totalEditedBooks:"3",institution:null}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,coeditorOne:null,coeditorTwo:null,coeditorThree:null,coeditorFour:null,coeditorFive:null,topics:[{id:"512",title:"Spectroscopy",slug:"chemistry-physical-chemistry-spectroscopy"}],chapters:[{id:"65184",title:"Introductory Chapter: Electron Paramagnetic Resonance",doi:"10.5772/intechopen.83028",slug:"introductory-chapter-electron-paramagnetic-resonance",totalDownloads:1190,totalCrossrefCites:0,totalDimensionsCites:0,hasAltmetrics:1,abstract:null,signatures:"Ahmed M. 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Electron paramagnetic resonance (EPR) has brought sufficient sensitivity and discrimination to observe free radical intermediates directly in many of these reactions. EPR is aided by an increased sensitivity in many cases and has made a much greater contribution by distinguishing among paramagnetic ions, odd molecules and free radicals.",signatures:"Betül Çalişkan and Ali Cengiz Çalişkan",downloadPdfUrl:"/chapter/pdf-download/62327",previewPdfUrl:"/chapter/pdf-preview/62327",authors:[{id:"199110",title:"Dr.",name:"Betül",surname:"Çalişkan",slug:"betul-caliskan",fullName:"Betül Çalişkan"},{id:"208732",title:"Dr.",name:"Ali Cengiz",surname:"Çalişkan",slug:"ali-cengiz-caliskan",fullName:"Ali Cengiz Çalişkan"}],corrections:null},{id:"62092",title:"Determination of Magnetic Anisotropy by EPR",doi:"10.5772/intechopen.78321",slug:"determination-of-magnetic-anisotropy-by-epr",totalDownloads:923,totalCrossrefCites:1,totalDimensionsCites:3,hasAltmetrics:0,abstract:"Electron paramagnetic resonance (EPR) is a powerful spectroscopic technique, perfectly suited for determining magnetic anisotropy terms in spin Hamiltonians. Although solid foundations of the EPR theory were established by Kubo and Tomita (KT) more than half a century ago, especially in the last couple of decades, we have witnessed a rapid progress in the field due to the occurrence of enhanced computational capabilities. In this chapter, we overview this progress by summarizing the basic concepts of EPR in exchange-coupled systems. The review builds upon the standard KT theory and the exchange narrowing picture, which is however only suitable at high enough temperatures and for systems with dimensionality exceeding one. We also summarize the predictions of more modern approaches, including exact calculations on finite spin clusters, the Oshikawa-Affleck effective-field theory for 1D systems, and the recently developed EPR-moments approach. Many illuminating examples of the applicability of different approaches are also provided.",signatures:"Andrej Zorko",downloadPdfUrl:"/chapter/pdf-download/62092",previewPdfUrl:"/chapter/pdf-preview/62092",authors:[null],corrections:null},{id:"62793",title:"EPR Methods Applied on Food Analysis",doi:"10.5772/intechopen.79844",slug:"epr-methods-applied-on-food-analysis",totalDownloads:1539,totalCrossrefCites:3,totalDimensionsCites:3,hasAltmetrics:0,abstract:"An overview of the different methodologies developed so far for the investigation of paramagnetic species in foods is presented. Electron paramagnetic resonance spectroscopy (EPR), also known as electron spin resonance spectroscopy (ESR), is the primary technique toward the development of methods for the exploration of EPR-sensitive species, such as free radicals, reactive oxygen species (ROS), nitrogen reactive species (NRS), and C-centered radicals and metal ions. These methods aim for: (a) quantification of radical species, (b) exploration of redox chemical reaction mechanisms in foods, (c) assessment of the antioxidant capacity of food, and (d) food quality, stability, and food shelf life. For these purposes, different radical initiations and detections have been used in foods depending on both the chemistry of the target system and the kind of information required, listed in: the induction of radicals by (a) microwave, UV, or γ-radiation; (b) heating; (c) addition of metals; and (d) use of oxidants.",signatures:"Chryssoula Drouza, Smaragda Spanou and Anastasios D. Keramidas",downloadPdfUrl:"/chapter/pdf-download/62793",previewPdfUrl:"/chapter/pdf-preview/62793",authors:[null],corrections:null},{id:"64373",title:"Modeling of Dielectric Resonator Antennas using Numerical Methods Applied to EPR",doi:"10.5772/intechopen.79087",slug:"modeling-of-dielectric-resonator-antennas-using-numerical-methods-applied-to-epr",totalDownloads:1049,totalCrossrefCites:0,totalDimensionsCites:0,hasAltmetrics:0,abstract:"This chapter presents an inclusive analysis of notable techniques carried out on modeling of dielectric resonator (DR)-antenna using numerical methods in last more than two decades. Dielectric resonator antenna (DRA) has created its individual existence in antenna engineering because of its captivating characteristics like; small size, low loss, high efficiency, wide bandwidth, three-dimensional design flexibility as compared to conventional antennas, etc. The DR antennas are being widely modeled using numerical methods nowadays. The triple-folded intention of this chapter is to: (1) give an overview on DRA modeling using single and hybrid numerical methods, (2) give a compressive review of notable numerical modeling researches carried out on DRAs and (3) give some favorable future concentration for the antenna researchers in order to apply the numerical methods on some innovative geometries of DRAs.",signatures:"Sounik Kiran Kumar Dash and Taimoor Khan",downloadPdfUrl:"/chapter/pdf-download/64373",previewPdfUrl:"/chapter/pdf-preview/64373",authors:[null],corrections:null}],productType:{id:"1",title:"Edited Volume",chapterContentType:"chapter",authoredCaption:"Edited by"},subseries:null,tags:null},relatedBooks:[{type:"book",id:"5451",title:"New Insights on Gamma Rays",subtitle:null,isOpenForSubmission:!1,hash:"0fe8c3174bbb6d68493d39220cdec7ca",slug:"new-insights-on-gamma-rays",bookSignature:"Ahmed M. 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\r\n\tNatural food items are still in utilization in this modern era of digitalization and technological advancements. Among various natural products, honey cannot be ignored, as it is a supersaturated solution of sugars along with complex chemical composition prepared by honeybees in the bee-hive. The complex chemical composition is dependent on beekeeping practices, climatic conditions, type of honeybee species, and botanical source. It is a complex mixture of numerous types of bioactive components such phenolic, enzymes, organic acids, peptides, vitamins, minerals, and antioxidants which have health-promoting potential against various types of diseases in the liver, gastrointestinal, cardiovascular, cancer, wound healing, and many other. It is considered the oldest medicine and is being studied as a therapeutic agent in modern medicine due to its inhibitory effect against microbial infections. Additionally, it acts as a natural preservative in many food applications. There is a plethora of literature that describes the physicochemical, geographical origin, and authentication of honey in this modern era. This book will aim to cover all the aspects that may affect the quality and composition of the honey starting from bee-keeping practices to end product utilization.
\r\n
\r\n\tThis book will also aim to include conventional and novel technologies such as spectroscopic, chromatographic, and non-thermal applications for the physicochemical characterization and authentication of honey and honey-based products. The clinical, pharmacological, and therapeutic potential of honey and its products are also intended to be included in this book.
",isbn:"978-1-80356-270-4",printIsbn:"978-1-80356-269-8",pdfIsbn:"978-1-80356-271-1",doi:null,price:0,priceEur:0,priceUsd:0,slug:null,numberOfPages:0,isOpenForSubmission:!1,isSalesforceBook:!1,isNomenclature:!1,hash:"60482dae5e08f5b22b0c7a2749cdfc02",bookSignature:"Dr. Muhammad Imran, Dr. Muhammad Haseeb Ahmad and Dr. Rabia Shabir Ahmad",publishedDate:null,coverURL:"https://cdn.intechopen.com/books/images_new/11802.jpg",keywords:"Honey Production, Beehives, Apiculture, Beekeeping Practices, Pharmacological Importance, Honey Efficacy, Honey Therapeutic Potential, Honey Characterization, Honey Functional Components, Honey Analysis, Honey Products, Modern Techniques",numberOfDownloads:null,numberOfWosCitations:0,numberOfCrossrefCitations:null,numberOfDimensionsCitations:null,numberOfTotalCitations:null,isAvailableForWebshopOrdering:!0,dateEndFirstStepPublish:"February 11th 2022",dateEndSecondStepPublish:"April 14th 2022",dateEndThirdStepPublish:"June 13th 2022",dateEndFourthStepPublish:"September 1st 2022",dateEndFifthStepPublish:"October 31st 2022",dateConfirmationOfParticipation:null,remainingDaysToSecondStep:"3 months",secondStepPassed:!0,areRegistrationsClosed:!0,currentStepOfPublishingProcess:4,editedByType:null,kuFlag:!1,biosketch:"A renowned researcher in the field of Food Science, Technology, and Nutrition. 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1. Introduction
Bell’s palsy is an acute, idiopathic, unilateral facial nerve paresis or paralysis of unknown cause. It leads to the partial or complete inability to voluntarily move facial muscles on the affected side of the face and may be occurring with equal frequency on the right and left sides of the face. Although typically self-limited, symptoms of Bell’s palsy may include oropharyngeal or facial numbness, disturbed taste on the anterior part of the tongue, impaired tolerance to ordinary levels of noise, mild pain in or behind the ear, significant oral incompetence, and an inability to close the eyelid, leading to potential eye injury. Clinically important improvement without intervention occurs within 3 weeks after onset of symptoms in 85% of patients and within 3–5 months in the remaining 15% [1]. Patients failing to show signs of improvement by 3 weeks may have suffered Wallerian degeneration of the facial nerve, leading to residual paresis and abnormal branching of regenerating axons, or may have an alternative diagnosis that requires identification by specialist examination or investigations. Among patients with Bell’s palsy, 71% obtained their normal facial muscle function [1]. Sequelae were slight in 12% of patients with Bell’s palsy, mild in 13%, and severe in 4% [1]. Incomplete recovery of facial expression may have a long-term impact on quality of life. Some patients with Bell’s palsy never recover despite treatment by pharmacotherapy and facial nerve decompression surgery. Physicians take the bold course of operation as a last resort. Contemporary reconstructive options include neurotization procedures (a new motor nerve is used to restore innervation to a viable muscle), contiguous regional muscle transfer (most commonly temporalis muscle transfer), and microsurgical free muscle transfer [2]. Additionally, some patients do not wish to undergo plastic and reconstructive surgery, and at present, there is no effective treatment for them [3]. Research on myogenin expression in the facial muscles following resection or compression of the facial nerve [4] indicated that facial muscle gene analysis might be a promising way to predict the outcome of facial palsy even at an early stage of the disease [4]. I thus performed a genetic analysis of the facial muscles in patients with Bell’s palsy and in rats after facial nerve resection and assessed its molecular biological aspects as a pathway to new treatments.
2. Materials and methods
2.1. Human specimens
The materials used to study the microarray analysis were obtained from the orbicularis oculi muscles of six Japanese patients with Bell’s palsy (females in their 60s). Three patients were judged to be House-Brackmann facial nerve grading system III (moderate dysfunction), and the other three were judged to be House-Brackmann facial nerve grading system V (severe dysfunction). Both groups had previously received nonsurgical conservative treatment using steroids and so on but had not undergone facial nerve decompression surgery. All the patients were treated with plastic and reconstructive procedures at 1.5 years after the onset of facial paralysis. Both groups underwent blepharoplasty of the superior eyelid for blepharoptosis on the affected side. They also underwent blepharoplasty on the healthy side for esthetic reasons. Biopsy materials were obtained from the palpebral part of orbicularis oculi on both the healthy side and the side with palsy. The microarray analysis of gene expression was performed using Affymetrix Human Gene 1.0 ST arrays (Affymetrix Inc., Santa Clara, CA, USA), and gene expressions were compared between the two sides. Changes of gene expression were defined as a palsy/healthy side expression ratio >2.0 or <0.5.
This study was approved by the local ethics review board (No. 149) at the Showa University Hospital. I conducted and had supervisory control of this study according to the Ethical Principles for Medical Research Involving Human Subjects in the Declaration of Helsinki. I provided all patients with detailed information about this study and obtained written informed consent prior to inclusion from both patients and doctors for participation in this study.
2.2. Rat specimens
Three male Slc: Wistar/ST rats weighing 300 g (12 weeks old) were used. The management of environmental variables of rats was as follows: (1) the room temperature range for rat housing between 21 and 23°C, (2) the humidity at the level of rat cages of 40–70%, (3) the room ventilation rates of about 15–20 air changes per hour, and (4) the light cycles of 12/12 hours light/dark. The animals were allowed to have food and water provided ad libitum until the end of the experiment.
Each animal was anesthetized with an intraperitoneal injection of 0.15 mg/kg of medetomidine hydrochloride, 2.0 mg/kg of midazolam, and 2.5 mg/kg of butorphanol tartrate and fixed on an experimental table in the prone position. The face was shaved and cleaned, and a skin incision was made to expose the extratemporal portion of the facial nerve bilaterally. On the nerve resection side (right side), the main trunk of the facial nerve was cut just distal to the stylomastoid foramen, forming a 7 mm gap in the trunk to avoid regeneration. In sham surgery group, the facial nerve on the opposite side (left side) was exposed without further manipulation. The rats were returned to the animal room after completion of these procedures.
The rats were sacrificed under deep anesthesia by intraperitoneal administration of pentobarbital (150 mg/kg) on the third postoperative week. A piece of orbicularis oculi muscle was obtained from each side and immediately immersed in RNAlater solution (QIAGEN N. V.; Venlo, Netherlands), for gene expression analysis. The microarray analysis of gene expression was performed using Affymetrix Human Gene 1.0 ST arrays (Affymetrix Inc., Santa Clara, CA, USA), and gene expression was compared between the two sides. Changes of gene expression were defined as a palsy/healthy side expression ratio >2.0 or <0.5.
Under the approval of the Ethics Committee of Nagoya City University Graduate School of Medical Sciences (No. H27M-74), the present study was conducted following the Guidelines for Animal Experimentation at the above institute. All efforts were made to minimize suffering and the number of animals used, as described in the experimental protocol.
3. Results
Table 1 summarizes the data from the three severities of facial nerve palsy (House-Brackmann facial nerve grading system III, V, and VI). Only 13 genes showed similar changes between patients with moderate dysfunction and those with severe dysfunction, and only one gene showed similar changes between patients with moderate dysfunction and rats with total paralysis. In contrast, 333 genes showed similar changes between patients with severe dysfunction and rats with total paralysis. The overall changes indicated that patients with moderate dysfunction differed from those with severe dysfunction and rats with total paralysis.
Table 1.
Comparison of changes in gene expression between the three severities of facial nerve palsy. Changes of gene expression were defined as a palsy/healthy side ratio > 2.0 or < 0.5. indicates that most genes in the category were downregulated. indicates that some genes in the category were downregulated. indicates that most genes in the category were upregulated. indicates that some genes in the category were upregulated. indicates that expression of genes in the category did not change. Numbers (mean values) on the right side of the arrows indicate the number of genes showing changes.
3.1. Patients with moderate dysfunction
A total of 174 genes showed changes, which was a relatively low number. Genes in the neuron category tended to show downregulation, while most genes showing changes in the muscle category were upregulated. Genes related to muscle components and genes involved in muscle movement were also upregulated. Only two energy production genes were upregulated, and both were important genes related to the glycolysis pathway. I did not find any large functional clusters except for these functional categories. Some genes involved in cell proliferation and cell division showed downregulation. However, genes linked to stress markers and apoptosis did not show upregulation (Table 1).
3.2. Patients with severe dysfunction
A total of 763 genes showed changes of expression. Among 59 genes with changes in the neuron category, 39 genes showed upregulation and 20 genes showed downregulation. Most genes showing changes in the muscle and energy categories showed downregulation, but some genes related to immunity, inflammation, and stress, in contrast, showed upregulation (Table 1).
3.3. Rats with total paralysis
A total of 1102 genes showed changes of expression. Among 47 genes with changes in the neuron category, 29 genes were upregulated and 18 were downregulated. Some genes linked to immunity, stress, and autophagy were also upregulated. Moreover, most genes showing changes in the inflammation category were upregulated. In contrast, most genes showing changes in the muscle and energy categories showed downregulation (Table 1).
4. Discussion
The total number of genes showing changes of expression (mean values for the patients) in the patients with moderate dysfunction was 174, compared to 763 in the patients with severe dysfunction. The total number of genes that changed in both groups was 25, but only 13 genes showed changes of expression in the same direction. Next, the total number of genes showing changes of expression (mean values for the patients and rats) in the patients with moderate dysfunction was 174 but 1102 in the rats with total paralysis. The total number of genes that changed in both groups was 19, but only one gene showed changes of expression in the same direction. These findings indicated that the condition of moderate dysfunction differed greatly from that of severe dysfunction in patients with facial nerve palsy and rats with total paralysis.
Considering these findings, I speculate that, if facial nerve conduction is reduced in moderate dysfunction, the orbicularis oculi muscle cannot function well and the patient presents with paresis. To improve this situation, regeneration of muscle tissue is promoted. Researchers reported that innervation is required for normal energy production in muscles [5]. Therefore, due to denervation, there was the decrease in energy production in muscles with paresis, but patients with moderate dysfunction had some energy production related to regeneration of muscle tissue. There was very little energy production or regeneration of the affected muscles because of the largely abolished facial nerve conduction in patients with severe dysfunction. Accordingly, the muscles innervated by the facial nerve did not show much regeneration, but the neurons themselves showed accelerated regeneration.
On the basis of these genetic findings, I suggest that neurorrhaphy and nerve grafting of the facial nerve are appropriate for patients with moderate dysfunction. These procedures will improve facial nerve conduction, leading to the increase in energy production for the regeneration of muscle tissue. However, there was little muscle regeneration and very low energy production in patients with severe dysfunction, although they showed acceleration of neuronal regeneration. These findings may explain why neurorrhaphy and nerve grafting of the facial nerve are unsuccessful if performed more than 1 year after the onset of facial palsy. Many authors have reported that recovery is better if the interval between injury to the facial nerve and repair surgery on the facial nerve is shorter [6, 7, 8]. Because improvement of facial nerve conduction is incomplete in patients with severe dysfunction, I consider that promoting the regeneration of muscle tissue and energy production is necessary. It is possible that some form of regenerative medicine, such as the use of induced pluripotent stem (iPS) cells, could be employed to improve muscle regeneration [9]. However, before such treatments become available for clinical use, I propose administration of pyruvate or mitochonic acid 5 (MA-5) as a practical way to promote muscle regeneration and energy production. Pyruvate plays a pivotal role in central carbon metabolism. Pyruvate is generated from several sources, including the end product of glycolysis, the oxidation of lactate, or as the transamination of alanine. Pyruvate is crucial for ATP generation in mitochondria and for driving several major biosynthetic pathways intersecting the citric acid cycle. In addition, it is well known that pyruvate can eliminate hydrogen peroxide by a nonenzymatic reaction to form acetate, carbon dioxide, and water [10]. This antioxidant activity of pyruvate may be also beneficial for patients with mitochondrial disorders, because the respiratory defects increase the leakage of reactive oxygen species from the mitochondria. Thus, administration of pyruvate restores the production of adenosine 5′-triposphate (ATP) via the glycolytic pathway. MA-5 targets the mitochondrial protein mitofilin at the crista junction of the inner membrane and could be a novel treatment for diseases associated with mitochondrial dysfunction [11, 12]. In Bell’s palsy patients with severe dysfunction, it seems that mitochondrial cytopathy develops with impairment of ATP synthesis. As this state is similar to that in various mitochondrial diseases, I consider that pyruvate therapy [13, 14] and the administration of MA-5 could be effective. I also propose neurovascular free muscle transfer as effective surgery for patients with severe dysfunction of facial palsy. Neurovascular free muscle transfer is one of the main reconstructive surgeries for established or long-standing facial palsy [15], but it also seems to be suitable for severe facial palsy based on genetic findings in this study, and I suggest that neurovascular free muscle transfer could be more effective than facial nerve neurorrhaphy with nerve grafting in patients with severe dysfunction.
Grading of facial function is necessary for evaluating and communicating the spontaneous course and the results of medical and surgical treatment of facial palsy [16, 17]. Several grading systems for the assessment of facial nerve function using gross (e.g., the House-Brackmann grading system) [16] or regional (e.g., the Yanagihara grading system) [18] scales have been proposed. In this study, patients with severe dysfunction who were judged as grade V by the House-Brackmann system also scored 8–14 points with the Yanagihara system. The clinical description in patients with severe dysfunction is barely perceptible motion, whereas that in patients with total paralysis (House-Brackmann grading system VI) is no movement. As these two clinical descriptions differ widely, I compared the changes in gene expression between patients with severe dysfunction and rats with total paralysis (Table 1). The total number of genes that changed in both groups was 403 and that of gene expression in the same direction accounted for around 83% (333 genes). Some genes linked to immunity, inflammation (most genes showing changes in rats), and stress were upregulated in both groups. In the neuron category, the number of upregulated genes tended to be higher than the number of downregulated genes in both groups. Moreover, in both groups, most genes showing changes in the energy and muscle categories were downregulated. As mentioned above, the condition of moderate dysfunction differed widely from that of severe dysfunction in patients with facial nerve palsy and rats with total paralysis, but the overall changes indicated that gene expressions in patients with severe dysfunction were similar to those in rats with total paralysis. In general, the molecular biological changes after neurotmesis are as follows: (1) nerve transection produces morphological changes in the neuronal perikarya known as chromatolysis or axon reaction, and the changes include swelling of the cell body, nucleolar enlargement, displacement of the nucleus to the periphery, and dissolution of Nissl bodies [19] and (2) axotomized neurons respond by upregulation of regeneration-associated genes in association with conversion of the neuron from a transmitting to a growth state [20]. Remarkable molecular biological changes after neurotmesis, as described above, lasted for 10–20 days. Rat specimens in this study were obtained on the third postoperative week. Therefore, the rat models in this study closely resembled patients with total paralysis (House-Brackmann grading system VI). Synthesizing these results based on molecular biological analyses, I suggest that clinicians treat patients with severe dysfunction (House-Brackmann grading system V) with the same treatment as for patients with total paralysis (House-Brackmann grading system VI).
5. Conclusions
I conclude that the gene expression in facial nerve palsy changes with the degree of facial nerve palsy. This study will aid in the development of new treatments and diagnostic/prognostic markers based on the severity of facial nerve palsy.
Acknowledgments
I thank Prof. Nobuyuki Mitsukawa for providing human specimens and Prof. Shingo Murakami and Dr. Akira Inagaki for providing animal specimens. I thank Dr. Yoshiyuki Takahara for helping in analyzing the DNA microarray and Ms. Ikuko Moriyama for assistance in preparing the manuscript.
Conflicts of interest
The author has no conflicts of interest to declare.
Ethics approval of research
The local Ethics Review Board of Showa University Hospital approved the study protocol (No. 149) according to the principles of the Declaration of Helsinki. All the patients were provided with detailed information about the study and provided written informed consent prior to their inclusion. I abided by the Ethical Principles for Medical Research Involving Human Subjects outlined in the Declaration of Helsinki. With regard to animal experimentation, the present study was conducted following the Guidelines for Institutional Animal Experimentation under the approval of the Ethics Committee of Nagoya City University Graduate School of Medical Sciences (No. H27M-74). I made every effort to minimize pain, discomfort for the animals and the number of animals used, as written in the experimental protocol.
Financial support and disclosure
This work was supported by the annual budget of Showa University for scientific research. I certify that the funding agencies had no involvement in the design, data collection, analysis, or interpretation of the results. The corresponding author had full access to all the data in the study and had final responsibility for the decision to submit for publication.
\n',keywords:"facial nerve palsy, facial muscle, orbicularis oculi, microarray analysis, gene expression",chapterPDFUrl:"https://cdn.intechopen.com/pdfs/64297.pdf",chapterXML:"https://mts.intechopen.com/source/xml/64297.xml",downloadPdfUrl:"/chapter/pdf-download/64297",previewPdfUrl:"/chapter/pdf-preview/64297",totalDownloads:1060,totalViews:89,totalCrossrefCites:0,totalDimensionsCites:0,totalAltmetricsMentions:0,impactScore:0,impactScorePercentile:30,impactScoreQuartile:2,hasAltmetrics:0,dateSubmitted:"July 17th 2018",dateReviewed:"October 10th 2018",datePrePublished:"November 5th 2018",datePublished:"May 29th 2019",dateFinished:"November 5th 2018",readingETA:"0",abstract:"Details of the molecular biological features of facial nerve palsy have not been widely reported in textbooks. I performed a genetic analysis of facial muscle specimens from Japanese patients with moderate (House-Brackmann facial nerve grading system III) and severe (House-Brackmann facial nerve grading system V) dysfunctions due to Bell’s palsy and rats, after facial nerve resection (total paralysis). Microarray analysis of gene expression was performed using specimens from both the healthy and affected sides, and gene expressions were compared. Changes in gene expression were defined as a palsy/healthy side ratio >2.0 or <0.5. I observed changes of gene expression; in particular, genes for muscle, neuron, and energy function showed changes with the severity of facial nerve palsy. This study may aid the development of new treatments and diagnostic/prognostic markers based on the severity of palsy.",reviewType:"peer-reviewed",bibtexUrl:"/chapter/bibtex/64297",risUrl:"/chapter/ris/64297",book:{id:"7131",slug:"selected-topics-in-facial-nerve-disorders"},signatures:"Hiroshi Moriyama",authors:[{id:"141619",title:"Prof.",name:"Hiroshi",middleName:null,surname:"Moriyama",fullName:"Hiroshi Moriyama",slug:"hiroshi-moriyama",email:"veloce@med.showa-u.ac.jp",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/141619/images/system/141619.jpg",institution:{name:"Showa University",institutionURL:null,country:{name:"Japan"}}}],sections:[{id:"sec_1",title:"1. Introduction",level:"1"},{id:"sec_2",title:"2. Materials and methods",level:"1"},{id:"sec_2_2",title:"2.1. Human specimens",level:"2"},{id:"sec_3_2",title:"2.2. Rat specimens",level:"2"},{id:"sec_5",title:"3. Results",level:"1"},{id:"sec_5_2",title:"3.1. Patients with moderate dysfunction",level:"2"},{id:"sec_6_2",title:"3.2. Patients with severe dysfunction",level:"2"},{id:"sec_7_2",title:"3.3. Rats with total paralysis",level:"2"},{id:"sec_9",title:"4. Discussion",level:"1"},{id:"sec_10",title:"5. Conclusions",level:"1"},{id:"sec_11",title:"Acknowledgments",level:"1"},{id:"sec_14",title:"Conflicts of interest",level:"1"},{id:"sec_11",title:"Ethics approval of research",level:"1"},{id:"sec_12",title:"Financial support and disclosure",level:"1"}],chapterReferences:[{id:"B1",body:'Peitersen E. Bell’s palsy: The spontaneous course of 2,500 peripheral facial nerve palsies of different etiologies. Acta Oto-Laryngologica. Supplementum. 2002;549:4-30'},{id:"B2",body:'Garcia R, Hadlock T, Klebuc M, Simpson R, Zenn M, Marcus J. Contemporary solutions for the treatment of facial nerve paralysis. Plastic and Reconstructive Surgery. 2015;135:1025e-1046e'},{id:"B3",body:'Holland J, Bernstein J. Bell’s palsy. BMJ Clinical Evidence. 2011;2011:1204'},{id:"B4",body:'Teraoka M, Hato N, Takahashi H, Komobuchi H, Sawai N, Okada M, et al. Myogenin expression in facial muscle following damage to the facial nerve. Acta Oto-Laryngologica. 2012;132:783-787'},{id:"B5",body:'Sato D, Shinzawa G, Kusunoki M, Matsui T, Sasaki H, Feng Z, et al. Effects of electrical microstimulation of peripheral sympathetic nervous fascicle on glucose uptake in rats. Journal of Artificial Organs. 2013;16:352-358'},{id:"B6",body:'Conley J, Baker DC. Hypoglossal-facial nerve anastomosis for reinnervation of the paralyzed face. Plastic and Reconstructive Surgery. 1979;63:63-72'},{id:"B7",body:'Gavron JP, Clemis JD. Hypoglossal-facial nerve anastomosis: A review of forty cases caused by facial nerve injuries in the posterior fossa. The Laryngoscope. 1984;94:1447-1450'},{id:"B8",body:'Kunihiro T, Kanzaki J, Yoshihara S, Satoh Y, Satoh A. Hypoglossal-facial nerve anastomosis after acoustic neuroma resection: lnfluence of the time of anastomosis on recovery of facial movement. ORL: Journal for Otorhinolaryngology and Its Related Specialties. 1996;58:32-35'},{id:"B9",body:'Masumoto H, Ikuno T, Takeda M, Fukushima H, Marui A, Katayama S, et al. Human iPS cell-engineered cardiac tissue sheets with cardiomyocytes and vascular cells for cardiac regeneration. Scientific Reports. 2014;4:6716. DOI: 10.1038/srep06716'},{id:"B10",body:'Nath K, Ngo E, Hebbel R, Croatt A, Zhou B, Nutter L. alph-Ketoacids scavenge H2O2 in vitro and in vivo and reduce menadione-induced DNA injury and cytotoxicity. The American Journal of Physiology. 1995;268:C227-C236'},{id:"B11",body:'Suzuki T, Yamaguchi H, Kikusato M, Hashizume O, Nagatoishi S, Matsuo A, et al. Mitochonic acid 5 binds mitochondria and ameliorates renal tubular and cardiac myocyte damage. Journal of the American Society of Nephrology. 2016;27:1925-1932'},{id:"B12",body:'Suzuki T, Yamaguchi H, Kikusato M, Matsuhashi T, Matsuo A, Sato T, et al. Mitochonic acid 5 (MA-5), a derivative of the plant hormone indole-3-acetic acid, improves survival of fibroblasts from patients with mitochondrial diseases. The Tohoku Journal of Experimental Medicine. 2015;236:225-232'},{id:"B13",body:'Tanaka M, Nishigaki Y, Fuku N, Ibi T, Sahashi K, Koga Y. Therapeutic potential of pyruvate therapy for mitochondrial diseases. Mitochondrion. 2007;7:399-401'},{id:"B14",body:'Kerr DS. Review of clinical trials for mitochondrial disorders: 1997-2012. Neurotherapeutics. 2013;10:307-319'},{id:"B15",body:'Takushima A, Harii K, Asato H, Kurita M, Shiraishi T. Fifteen-year survey of one-stage latissimus dorsi muscle transfer for treatment of longstanding facial paralysis. Journal of Plastic, Reconstructive & Aesthetic Surgery. 2013;66:29-36'},{id:"B16",body:'House JW, Brackmann DE. Facial nerve grading system. Otolaryngology and Head and Neck Surgery. 1985;93:146-147'},{id:"B17",body:'House JW. Facial nerve grading systems. The Laryngoscope. 1983;93:1056-1069'},{id:"B18",body:'Yanagihara N. Grading of facial palsy. In: Fisch U, editor. Proceedings of the Third International Symposium on Facial Nerve Surgery. Zurich: Kugler Medical Publications; 1976. pp. 533-535'},{id:"B19",body:'Kreutzberg GW. Microglia, the first line of defense in brain pathologies. Arzneimittel-Forschung. 1995;45:357-360'},{id:"B20",body:'Boyd JG, Gordon T. Neurotrophic factors and their receptors in axonal regeneration and functional recovery after peripheral nerve injury. Molecular Neurobiology. 2003;27:277-324'}],footnotes:[],contributors:[{corresp:"yes",contributorFullName:"Hiroshi Moriyama",address:"veloce@med.showa-u.ac.jp",affiliation:'
Department of Anatomy, Showa University School of Medicine, Shinagawa-ku, Tokyo, Japan
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1. Introduction
Every cell is defined by its membrane. This amphiphilic molecular matrix is highly organized and complex in terms of its lipid and protein components. Ion channels have evolved to mediate ion transport throughout membranes always in favor of electrochemical gradients from free-living bacteria to mammal neurons [1, 2]. In doing so, these membrane proteins are part of complex physiological networks which include signal transduction processes, cellular communication, or the propagation of electrical signals [3]. The voltage-gated ion channel (VGIC) superfamily comprises dozens of variations on a common theme—(i) a voltage sensor domain (VSD) and (ii) a pore domain (PD) [4]. This modular architecture has in turn evolved into activation mechanisms as diverse as the detection of changes in the potential across the membrane, the binding of diverse chemical ligands, local membrane stretching, or subtle changes in temperature or the pH. In consequence, those physical-chemical variables are often interrelated modulating the ion channel gating but not clearly defined as exclusive stimuli for a determined protein [5]. In voltage sensing, the VSD performs important conformational rearrangements moving through the membrane-electric field and coupling this motion to the opening of the permeation pathway at the PD. To do this, four transmembrane segments (S1–S4) at the VSD respond sensing the electric field by translocating the so-called gating charges and by reorganization of the dipole moments into an aqueous crevice around the S4 segments, so that at any membrane potential, the charged side-chains of basic residues (mainly Arg and Lys) are essentially both hydrated and ionized either above or below the plane of the lipid bilayer (i.e. depolarized or hyperpolarized, respectively) [6].
In that sense, the VSD is clearly a mobile and intrinsically flexible element. A more detailed analysis of this mobility has revealed the relative flexibility of the different regions into this domain and clearly demonstrate that helices S1, S2, and the N-terminal part of S3 (S3a) are relatively more static than the so-called VSD paddle (S3b-S4) which loop linker show enhanced flexibility at higher temperatures in molecular simulations [7]. In those in silico studies, it is also evident that the segment S4 undergoes hinge bending and swiveling about its central axis, motion facilitated by the conformational instability of the S3a helix [7, 8]. The intrinsic flexibility of the S3a region facilitates movement of the segment S3b-S4, which in turn exhibits an even higher flexibility profile due to its composition rich in residues with small side-chain (Gly, Ser, Thr) and basic residues (Figure 1). Notably, these predictions have been experimentally confirmed elsewhere [9, 10] and some reports also indicate that abnormal S4 movements cause pathological effects related for example to the development of epilepsy [11]. Therefore, it is becoming increasingly clear that the VSD is a flexible dynamic structure with evident relevance in physiological disorders.
Figure 1.
Flexibility plot for the VSD of Kv1.2-Kv2.1 paddle chimera (PDB code: 2r9r) calculated using the method previously reported by us [5]. a. Cartoons showing the hyperpolarized (left) and depolarized (right) conformations of the VSD. b. Plots showing B-factors normalized to a Gumbel distribution according to our previous studies. Segment S3b-S4, involved in channel activation and the electromechanical coupling exhibits higher flexibility than the rest of the voltage sensor (S1–S3a).
The mechanisms of gating in ion channels have been intensively studied. On activation, outward S4 motion is associated with specific interactions with conserved negative countercharges (Asp and Glu) in transmembrane segments S1, S2, and S3 by forming sequential salt bridges with the positively charged residues in S4 inside an aqueous pore (Figure 2). Such interactions facilitate the translocation of the S4 segment in an energetically unfavorable membrane environment promoting the sequential salt-bridge formation and the electromechanical activation of the S4-S5 linker, which directly couples voltage sensor movement to the activation gate [12]. These negative countercharges are well-conserved in S1, S2, and S3 transmembrane segments in Kv channels (Figure 3). Besides, several VSD countercharge mutations associated with disease phenotypes including neural, cardiac, or skeletal muscle disorders have also been identified [14]. Despite channelopathies often affect ion channel gating, many of these pathologies have yet to be functionally or biophysically characterized. In this regard and given the diverse physiological and pathophysiological functions played by members of the VGIC superfamily, the VSD becomes a promising target for rational drug design.
Figure 2.
The gating charge transfer center (CTC) in the voltage sensors of Kv channels. a. Ribbon representation of the four segments (S1–S4) making one VSD of the human ether-a-go-go-related gene (hERG) channel (PDB code: 7cn0). b. Close-up view of the CTC highlighting the gating charges on the S4 segment. Side-chains of the positively charged residues on S4 (labeled as R and K) and negative residues D456 and D460 interact forming salt bridges. The hydrophobic residue F463 controls the energy barrier of the final gating transition. Figures containing structures were prepared with Pymol (http://www.pymol.org/).
Figure 3.
Sequence logos from the three main subfamilies of voltage-gated potassium channels using the webserver WebLogo (http://weblogo.threeplusone.com/). The bars below the sequence logos represent the extent of transmembrane segments S1–S4. The consensus sequences generated are represented statistically, showing the relative conservation of each residue at that position. The height of each letter in every position indicates the maximum theoretical entropy for protein sequences (measured in bits) [13] which is determined by the number of aligned sequences and the degree of ambiguity in the alignments for each residue. Blue stars indicate basic residues involved in voltage sensing on S4. Green circles indicate conserved negative countercharges in S2 and S3. Red hexagon depicts a well-conserved aromatic residue that controls the transfer of the more inner gating charge, shaping the electric field inside the voltage sensor. Conserved residues addressed in this study are color-coded as: Red (hydrophobic); green (acidic); blue (basic); orange (small side-chain); pink (flexible side-chain); and black (rigid side-chain).
2. The voltage sensor domain as a pharmacological target
There are many reports on the interactions of different intracellular ligands with ion channels and particularly important is the well-understood interaction of ligands with the cytosolic tail domain (CTD) in large-conductance calcium-activated potassium channels (BKCa), which contain several binding sites. Also relevant are the studies of the interaction of cGMP or cAMP with the cyclic nucleotide-binding domain (CNBD) in cyclic nucleotide-gated (CNG) and hyperpolarization-activated (HCN) channels. Structural and functional information has shown that frequently the ligand-binding sites in those channels are clustered located at the interface between the cytosolic domain and the VSD, acting synergistically to activate the gate at the PD [15, 16]. In other studies, ligands have been found directly coupled to the VSD influencing the channel activation, opening, closing, or inactivating the pore, such as some protein toxins from tarantula do [17, 18] or the binding of vanilloids, monoterpenoids, and related compounds to the S1–S4 domain in the transient receptor potential (TRP) channels [19].
From a structural perspective, the study of interactions between specific chemical ligands and the VSD in ion channels opens the possibility to rationally design both agonist and antagonist drugs. Let us have a look at three specific cases—(1) the voltage- and lipid-gated potassium channel KCNQ2 (Figure 4), (2) the cold/menthol activated TRPM8 channel (Figure 5), and (3) the capsaicin receptor TRPV1 (Figure 6). Studies on the KCNQ2 (Kv7.2) potassium channel show that the aromatic amide ztz240, a derivative of niclosamide, binds to the open configuration of the VSD. This interaction directly couples such a chemical ligand with a binding pocket of 170 Å3 located between some specific residues at segments S2 (Glu130, Ile134, Phe137) and S4 (Arg207 and Arg210), i.e. precisely in the gating charge pathway of this ion channel [20]. This raises the possibility to design drugs using the channel gating pore in voltage-dependent channels as a therapeutic target [21]. In this case, ztz240 and some derived chemotypes have demonstrated important anti-epileptic activity, which might be valuable for the treatment of epilepsy (see below). Remarkably, this interaction in the gating charge pathway of KCNQ2, considering the induced-fit model, demonstrates that this pocket may accommodate different activators [20].
Figure 4.
Structure of the human Kv7.2 (KCNQ2) channel (PDB accessions codes 7cr0 (apostate) and 7cr1 (in complex with ztz240). a. Ribbon representation of side view showing the VSDs exposed to the lipid bilayer (not shown here). b. Surface representation showing the ligand-binding pocket as a box. c. the unliganded structure of the VSD (highlighted in pale green) is superimposed with the one in complex with ligand (highlighted in smudge green). d. Three-dimensional stick representation of the Kv7.2 pocket in complex with ligand ztz240 (dark brown). The distances traveled by the side-chain conformational rotamers are shown as dashes. The overlapping residues correspond to the side-chains involved in ligand binding.
Figure 5.
Structure of the TRPM8 ion channel from the collared flycatcher (Ficedula albicollis) (PDB codes 6bpq (apostate) and 6nr3 (in complex with icilin, PI(4,5)P2, and Ca2+). a. Ribbon representation of side view. b. Surface representation showing the ligand-binding pocket as a box. c. The unliganded structure of the VSLD is highlighted in light blue and superimposed with the one in complex with icilin (semi-dark blue). d. Overlay of both structures to visualize the side-chain conformation changes (see Figure 3 for details).
Figure 6.
Structure of the TRPV1 channel from rat (PDB codes 7lp9 (apostate, 4°C), 7lpe (in complex with capsaicin, 48°C), and 7lpa (in complex with capsaicin, 4°C). a. Side view of the tetramer in ribbon representation. b. Surface representation showing the ligand-binding pocket as a box. c. The unliganded structure of the VSLD is highlighted in light orange and superimposed with the one in complex with capsaicin (bright orange). d. Overlay of structures at 4°C (apostate) and 48°C (in presence of capsaicin) to visualize two different rotamers by residue (see Figure 3 for details). Inset: Superposition of Arg557 side-chain obtained at 4°C for apo- and holo-structures.
In the case of TRPM8, an analog binding pocket has been described as highly adaptable to accommodate diverse chemical structures in distinct orientations. Both agonists and antagonists are dynamically recognized in this promiscuous pocket making the whole S1–S4 domain conformationally dynamic and transmitting these rearrangements to the TRP helix, but without inducing important changes in its overall structure [22]. Menthol, the main compound of mint, is the clue activator to understand how TRPM8 channels are ligand-activated. It binds to the cavity formed between S1 and S4 by a so-called “grab and stand” mechanism. The hydroxyl group of menthol works as a hand to specifically grab with Arg842 (segment S4) through a hydrogen bond, while its isopropyl “legs” stand on residues on S4 through electrostatic interactions. Thus, menthol binding induced widespread conformational rearrangements in the S1–S4 domain which open the S6 bundle gate to allow ion permeation [23].
On the other hand, since TRPV1 channels participate in several pathways of neuronal inflammatory signaling, it also represents an attractive therapeutic target for the treatment of neuroinflammation, neurodegenerative diseases, and chronic pain. Feng et al. [24] have studied diverse diarylurea compounds by molecular docking and dynamics, finding that specific residues located in the interface between the VSD and the PD are implicated in several van der Waals interactions. Particularly important are residues Tyr511, Leu518, Leu547, Thr550, Asn551, Arg557, and Leu670. Besides these observations, residues at the base of the interface between the VSD and the PD (segments S3, S4, S5, and the S4-S5 linker) are important binding sites for N-(3-fluoro-4-methylsulfonamidomethylphenyl)urea. Docking analysis of this compound with human TRPV1 has revealed that hydrogen bonding and π–π interactions with Tyr511 (segment S3) and hydrophobic interactions with two pockets in the S3 and S4 segments (residues Met514, Leu515 and Leu547, Thr550, respectively) are critical for its activity. Flexible docking studies have also revealed that N-benzyl phenylsulfonamide derivatives of 2-(3-fluoro-4- methylsulfonamidophenyl)propanamide specifically bind to the same pockets, being again critical for the potent activity of these antagonists [25, 26]. Notably, conformational analyses have revealed that the S1–S4 domain in TRPV channels remains relatively static during opening [27, 28, 29].
These three examples are mechanistically different, but they all share something in common, and this is the specific association of their respective ligands at the VSD, as well as their direct association with the potential difference across the membrane. However, even though TRP channels have frequently been treated as strictly ligand-dependent, it is increasingly clear that their voltage sensitivity could be underestimated [30]. These reports support the idea that the increasingly available detailed structural information, as well as detailed functional studies, greatly simplifies the search for chemical modulators with agonistic or antagonistic action. In consequence, the identification of potential ligand-binding sites in the VSD makes the rational design of new drugs, the goal of several research efforts.
2.1 Side-chain flexibility and ligand accommodation
Proteins are intrinsically flexible. This property derives from the two bonds associated with the carbon α (Cα), which can freely rotate and contribute to the flexibility of the main backbone. The torsion angles Phi (Φ) and Psi (ψ) represent the rotation around the Cα-N bond and the one around the Cα-carbonyl bond, respectively. However, this rotational capacity also depends on the steric and conformational effects of the associated side-chains. In these terms, one classical structural parameter to estimate the mobility of each atom into a protein structure is the so-called B-factor, which reflects the degree of thermal motion and static disorder. This parameter, also called the Debye−Waller factor, represents the atomic displacement of the macromolecule and is used in protein crystallography to describe the attenuation of X-ray or neutron scattering caused by thermal motion, which reflects the uncertainty in atom positions [31, 32]. Therefore, proteins are intrinsically rigid or flexible ultimately based on their primary sequence.
From this perspective, in addition to their known physical and chemical properties, if their relative location parameters are considered, amino acids can also be classified in terms of their contribution to the flexibility of a given segment within a protein. The amino acids that are considered rigid generally consist of those that exhibit bulky side-chains, generally cyclic or aromatic, those that have heavy heteroatoms, and are generally hydrophobic. On the other hand, amino acids considered flexible are those having polar side-chains, have charges, or whose side group is only a proton, i.e. glycine [33]. Proline deserves a separate discussion, as this amino acid has been considered both rigid and flexible in terms of its kinking effect on alpha helices [34].
Typically, flexibility in proteins has been visualized in terms of local and global motions, which include—(i) the multiple conformations that a certain residue can acquire in the polypeptide chain, (ii) local-scale fluctuations in the conformation of the side chains with respect to the backbone, and (iii) massive movements of subdomains with respect to another part of the protein [35]. In this last regard, a pioneer study of protein crystal structures shows that intrinsic flexibility can be distinguished in terms of hinge motions and shear displacements between close-packed segments of the protein [36]. It is becoming clearer that studying protein flexibility and the multiple side-chain conformations during molecular docking is very relevant since it may contribute to a favorable change in the Gibbs binding free energy by optimizing the van der Waals interactions between the protein and the ligand. This favors a change in enthalpy and minimizes the decrease in entropy [37, 38], albeit protein flexibility also depends on several other factors, including heat capacity, conformational entropy, salt bridge networks, electrostatic interactions, and the hydrophobic effect [39]. In any case, the study of side-chain flexibility in ion channels and how it contributes to ligand accommodation could be critical to understand molecular recognition events and predict ligand binding. This could open novel therapeutic strategies for the treatment of diverse neuropathic disorders.
2.2 Three cases of study: Kv7.2, TRPM8, TRPV1
Since flexible regions in proteins can be predicted from the primary sequence through the evaluation of the normalized B-factor for a determined structure [40], we have implemented an easy algorithm in Excel based on the procedure carried out by Smith and cols. [32, 33]. In general terms, B-factor normalization, Bn, depends on (1) the atomic thermal factor, B, reported on the PDB, (2) the sample mean value of B-factors, Bm, for a dataset of protein structures, and (3) the standard deviation of the sample distribution of such factors, Bσ, for a determined structure [41]. In sum, normalized B-factors are indicative of each local residue flexibility that can be calculated as:
Bn=B−BmBσE1
Based on these theoretical principles, we implemented an algorithm to predict local side-chain flexibility, which correlates the composition of amino acids in a protein sequence in the context of its N- and C-terminal neighbors. The program assigns a weighted normalized B-factor value based on a stiffness classification for each amino acid, in accordance with previously published results [33]. This software, so-called FlexiProt, includes Trp, Tyr, Phe, Cys, Ile, Val, His, Leu, and Met as rigid amino acids and the rest of them, i.e. Gly, Thr, Arg, Ser, Asn, Gln, Asp, Pro, Glu, and Lys as flexible. The program incorporates a graphical generator of local flexibility profiles, based on primary sequence, to help the user better visualize this disorder parameter for its subsequent structural evaluation. Flexiprot is friendly and interactive since although it runs automatically, it allows at all times the possibility of evaluating local subsequences for a better prediction of the internal flexibility parameter, based on structural aspects associated with the theoretical degrees of freedom of the side-chains.
Through this type of sequence analysis, we show in Figure 7 the local flexibility profiles of three distinct channels for the segments S3 to S4—(1) human KCNQ2 (hKv7.2), (2) mouse TRPM8 (mTRPM8), and (3) rat TRPV1 (rTRPV1). As in the Kv1.2-2.1 paddle chimera (Figure 1), in these three cases, local flexibility for segment S4 is always higher than the one for segment S3. However, the profile of the S3 segment in the TRPV1 channel is significantly stiffer than the other two, which have similar flexibility profiles for the same segment, although the S4 segment of the voltage-dependent channel Kv7.2 is considerably more flexible compared to their thermosensitive counterparts. This notorious flexibility is mainly determined by the highly conserved Arg residues, responsible for transporting the gating charges in the voltage sensor during the activation mechanism of these proteins [5]. Considering the new structures available for this channel in the presence of the ztz240 modulator, whose binding site is precisely in the intimacy of the voltage sensor, it becomes interesting to analyze the role of side-chain flexibility for each of the interacting residues and that has been mentioned elsewhere [20, 42]. Figure 4 show this interaction in two conformational states for the VSD of the Kv7.2 channel, in the absence and presence of the state-dependent modulator ztz240. For a segment of 145 residues that encompass the integrity of the VSD, a root-mean-square deviation (RMSD) of 1.159 Å is indicative of a fine accommodation for this drug without representing a significant conformational change of this protein domain. It is clearly noted that the intrinsically flexible residues Arg207 and Arg 210 at the S4 segment undergo an important conformational rearrangement that allows the ligand to be adequately accommodated through van der Waals interactions. The analysis of the structures also indicates that these residues are displaced 3.0 and 3.3 Å respectively. Another important residue, implicated in the potentiation of the activity of ztz240 is Glu130, an amino acid considered even more flexible than Arg [33], which is found as a countercharge in the S2 segment and whose side group moves 2.4 Å during the interaction. In contrast to these data, two other amino acids also important for the interaction, Ile134 and Phe137—amino acids of a rigid nature—show a rearrangement of 2.3 Å and 1.8 Å, respectively. These data suggest that the significant local flexibility of the S4 segment in this channel strongly contributes to ligand accommodation with minor effects on the large movements that the VSD experience during activation and that some of the main residues interact with this ligand move in a range of 1.8–3.3 Å.
Figure 7.
Predicted flexibility for segments S3 and S4 in human Kv7.2, TRPM8 (mouse), and TRPV1 (rat). Flexibility (defined by B-factor values) using the FlexiProt algorithm according to Ref. [5] shows a higher flexibility profile for segment S4 compared to S3. Predictions also indicate that the three channels follow the flexibility ranking TRPV1 < TRPM8 < Kv7.2. Asterisk indicates the start of the first turn of the α-helix at the N-terminal part of segment S3a. mBf: mean B-factor.
In TRPM8, a channel described also as sensitive to voltage [43, 44], a similar effect to Kv7.2/ztz240 is observed. According to recent structural studies of this channel, icilin, a compound derived from tetrahydropyrimidine-2-one and more potent than menthol as the agonist, binds to the voltage-sensor-like domain (VSLD) mainly through van der Waals interactions to residues Tyr745 (S1), Glu782 (S2) Asn799 (S3), Asp802 (S3), Arg841 (S4), and His844 (S4) [28, 45, 46]. Analogously to that seen in the Kv7.2 channel, the significant flexibility exhibited by the S3 and S4 segments in the TRPM8 channel contributes to a fine accommodation of icilin through conformational rearrangements of these amino acids in a range from 2 to 4.6 Å (Figure 5D). These displacements occur in the context of an RMSD of 0.89 Å over 123 Cα atoms which integrate the VSLD of this cold-sensitive channel. Similarly, the interaction of the antagonist TC-I 2014 in the same cavity of the VSLD [28] induces small rearrangements of the corresponding side-chains implicated in ligand sensitivity, with displacements of around 1–3 Å and an average RMSD of 0.427 Å (data not shown). Taken together, these observations suggest that the high flexibility profile in the S3 and primarily the S4 segments of these transmembrane domains facilitates a fine repositioning of the participating side-chains, which are implicated in ligand accommodation.
The case of the transient receptor potential vanilloid subtype 1 channel is slightly different. Figure 6 shows the interaction of capsaicin with the VSLD of TRPV1. Thanks to the recently released structural data of TRPV1 channels in presence of this ligand, a more detailed exploration of such interactions as a function of the associated local flexibility contribution of the VSLD contributes to a better understanding of this process. For a segment of 166 residues encompassing the whole VSLD and part of the TRPbox, an RMSD of 0.63 Å suggest an almost null conformational change for this part of the protein in the course of the closed-to-open transition during the ligand interaction, as it has been previously reported [25]. In this case, residues Val518, Met547, Thr550, and Asn551 move their side-chains less than 1 Å when they interact with capsaicin, whereas Tyr511 and Arg557 experience a significant displacement of 7.8 Å and 5.1 Å, respectively. These observations are consistent with the low predicted local flexibility for segment S3 in this channel (Figure 7, Table 1) [5]. Furthermore, they are also in good agreement with the vision that the VSLD acts as a rigid body during TRPV1 activation [25].
Flexibility parameters for the studied channels upon ligand interaction.
mBf, mean B-factor (1/mBf).
Our analysis shows that in this case, the low flexibility profile of the S3 segment contributes to creating a rigid crevice. This structure accommodates the catechol/vanilloid ring of capsaicin at the base of the VSLD where the bulky side-chain of Tyr511 residue rearranges with a displacement of almost 8 Å during a transition from 4 to 48°C. It is very significant that this tyrosine, which frequently is classified as a rigid side-chain with low conformational entropy, in the context of the structure of this channel, carries out a significant rearrangement even greater than Arg557, which has been frequently quantified as much more flexible [33, 47]. Besides, the side-chain of Arg557 at S4 undergoes a conformational rearrangement of 5.1 Å during the interaction but an almost null displacement (0.8 Å) if this is carried out at 4°C (Figure 6D, inset). Indeed, despite its low flexibility, tyrosine has been considered very effective for mediating molecular recognition maybe because changing the orientation of its side-chain from gauche negative (g−) to trans (t) conformation is equivalent to moving the hydroxyl group around 9 Å, which is the length of an average drug molecule [48, 49]. On the other hand, the motion of Arg557 is associated with the formation of a hydrogen bond with the Glu570 residue on the S4-S5 linker, leading to its swivel [50]. This also confirms that arginine often participates in molecular recognition events. The terminal positively charged guanidinium group of this residue affords multiple geometries due to its long side-chain can retain substantial residual conformational entropy occupying several rotameric states, while maintaining specific interactions through its charged functional group [51]. In sum, we hypothesize that, in contrast with the mechanism dependent on the large local (S3–S4) flexibility of the voltage-dependent Kv7.2 channel or the cold/menthol-activated TRPM8 channel, these large conformational changes in specific residues compensate for the low mobility that the whole transmembrane domain (i.e. the VSLD), as a rigid body, undergoes during TRPV1 activation.
3. Side-chain flexibility and the dynamic nature of protein-ligand interactions
Despite the large increase in deposition of crystallographic, NMR, and cryo-electron microscopy structures in recent years, little dynamic information regarding the conformational degrees of freedom of protein structures is currently available. In silico local flexibility theoretical prediction together with molecular dynamics algorithms are likely to be useful in helping to solve this limitation. Diverse computational strategies have been developed to explore the side-chain rotameric states as a function of the primary sequence, backbone structure, and ligand interaction by molecular docking in specific protein motifs [52, 53, 54]. Besides, the prediction of protein flexibility [32, 33, 40, 41], as well as its identification and visualization [55], have been a constant goal in protein research. Side-chain flexibility represents an intrinsic property of amino acids, as it correlates with configurational entropy differences and indeed is related to the generation of dynamic rotamers, which are defined as a particular combination of side-chain dihedral angles [38].
Given the dynamic and multifactorial nature of flexibility in proteins, trying to predict the binding mode of any ligand is an inspiring challenge. However, the use of predictive tools, dynamic simulations, and specific experimental tests will facilitate a better understanding of the molecular mechanisms underlying ligand-dependent modulation of ion channels. This could be of great impact on the rational design and discovery of novel drugs. Therefore, in the case of the study of the VSD as a ligand-binding motif, side-chain flexibility is especially relevant and must be always considered in light of the induced-fit model and conformational selection mechanisms [56]. In these terms, since side-chain and also frequently the backbone are subject to rearrangements upon ligand interaction (see our previous analysis above), we suggest that any experimental approach to develop novel drugs should be designed from the perspective of a dynamic target. In this sense, the study by Li and cols. is very relevant since they identify a hydrophobic pocket inside the charge transfer center (CTC) of the Kv7.2 channel which can accommodate different chemical ligands [20]. This enables such openers to regulate ion channel activation and offers new therapeutic strategies for the treatment of several hyperexcitability disorders, such as epilepsy and neuropathic pain. Since the VSD exhibits important conformational freedom during the gating process, it is important to note that this class of ligands preferentially binds to specific conformational states. The compound ztz240, for example, is accommodated to a hydrophobic pocket only when the VSD is in its activated conformation. This interaction stabilizes the activated state of the channel, thus contributing to its antiepileptic activity [57]. Therefore, it is conceivable to consider the so-called gating pore as an important target for ion channel research given its potential adaptability to new openers or inhibitors.
In the Figure 8 included at the end of this study, the workflow for the development of drugs with therapeutic potential is shown sequentially. In silico and structural studies, from the perspective of the “induced fit” model and the “conformational selection” hypothesis [58, 59], both contribute to a better understanding of the dynamic aspects of the protein/ligand interactions. In these terms, the role of side-chain flexibility becomes pivotal, and methods to predict it, such as the one performed herein, as well as methods to visualize it, such as those reported elsewhere [55] are indispensable analysis tools. By the appropriate selection of chemical candidates with pharmacological potential, ion channels with defined mutations can be experimentally evaluated, shedding some light on the involvement of specific residues in ligand accommodation and their effects on voltage sensor regulation. Furthermore, thanks to the correct study of the flexibility profiles for a given segment, it is also possible to evaluate the nature of these interactions, providing additional information about the degrees of freedom necessary for an adequate ligand accommodation. With this background, experimental testing in animal models and eventual clinical studies becomes an achievable goal for the treatment of neurological disorders and problems of acute pain.
Figure 8.
Compounds that act on the voltage sensor could be a good alternative for the development of new analgesic drugs and provide a complement to pain therapy. After synthesis of a compound with pharmacological potential, ion channel mutagenesis (1) and associated electrophysiological tests (2) are performed. The study of the activation/inactivation properties of ionic channels with therapeutic interest (3) is decisive for establishing correlations between the adaptability of the molecular target and the candidate drug (4). Considering side-chain intrinsic flexibility and the degree of pocket disorder during these molecular recognition events allows the identification of residues crucial for drug activity. Finally, the new active compounds are tested for their in vivo validation using animal models (5). This strategy could be applied to the discovery of several modulators capable of dealing with diverse neurological disorders (6).
From this perspective, the predictive analysis of local flexibility that we have performed here on three different ion channels clearly shows how the characteristic ligands of each protein are accommodated in the binding sites generating important conformational changes in the side-chains of specific residues. In a very revealing way, we found that the Kv7.2 channel and the TRPM8 have a VSD and a VSLD with high S3-S4 flexibility profiles (mBf of 1.44/1.48 for S3 and 1.68/1.59 for S4, respectively) (Table 1). These domains show small local conformational changes according to the corresponding RMSD values calculated (1.16 Å and 0.89 Å respectively), while on the other hand, a channel such as TRPV1, whose flexibility profile is rather rigid (mBf = 1.39 for S3 and 1.55 for S4) exhibits a still minor conformational change (RMSD = 0.63 Å for the equivalent segment) during the interaction with its specific ligand. Likewise, the conformational changes that we observe in the participating side-chains are also revealing, since the rotamers generated during the ligand interaction in flexible VSDs (Kv7.2 and TRPM8) are the result of rotations less than 3 Å on average, while in the case of the rigid S1-S4 segment of the TRPV1 channel, the conformational changes of the side-chains are less than 1 Å but two residues, in particular, Tyr511 (S3) and Arg557 (S4), undergo rotations of 7.8 Å and 5.1 Å, respectively, which suggest a different mechanism for ligand accommodation. This is even more revealing when it is considered that the conformational changes observed in the side-chain of Arg557 were obtained at 48°C [48] while the conformational rotamer for that residue at 4°C is less than 1 Å and that corresponding to Tyr 511 is even higher (8.2 Å) with a side-chain angle rotation of ~101°, which also suggest that motion of this residue is critical for ligand binding (Figure 6D).
After this analysis, we speculate that two different mechanisms for ligand accommodation in ion channels exist, which seem to be dependent on the conformational freedom of the VSD. These mechanisms could be interpreted as VSDs that have higher degrees of freedom, i.e. flexible and more prone to fine induced-fit mechanisms, which adapt better to the ligand through small displacements of multiple participating side-chains. On the other hand, more rigid VSDs follow the classical lock and key model for enzyme-substrate interactions, in which the ligand is accommodated directly but with important conformational changes in certain very specific residues. The conformational freedom of these specific residues would compensate for the low mobility observed in the rest of the structure.
4. Conclusions
Flexible regions in proteins are critical elements for the recognition of macromolecular interactions and induced molecular flexibility is essential to understand the principles of molecular recognition between ligand and receptor. However, the nature of side-chain flexibility is elusive and dynamic processes involving this flexible component are among the most difficult to characterize. Given its direct participation in the activation of voltage-dependent channels, the voltage-sensing domain is a very attractive target from the therapeutic point of view. As side-chain flexibility represents an intrinsic property of amino acids which is correlated with configurational entropy differences, it is now known that rotamer changes in specific residues during ligand interaction are finely synchronized [38]. Our analysis has confirmed this claim. According to our predictive algorithm, the local flexibility in S3–S4 segments which are implied to ligand binding in three different channels, correlated well with the adaptability of specific residues through the generation of side-chain rotamers during each interaction. However, what is intriguing is the fact that segments exhibiting high flexibility profiles (i.e. Kv7.2 and TRPM8) are correlated with small-scale changes and the generation of side-chain rotamers that are more homogeneously and subtly accommodated among the participating residues during ligand binding, while those which are slightly more rigid (i.e. TRPV1) remain practically immobile during the interaction, except for one or two residues that undergo a very pronounced conformational rearrangement to accommodate the drug. Since it is assumed that these new conformations are energetically favorable states [60], in terms of drug design these observations might not be trivial when considering the induced-fit model [58, 59] in combination with the conformational selection hypothesis [61]. In agreement with them, the dynamic binding of drugs to a specific protein target may lead to chemoselectivity, high ligand affinity as well as the favoring of long residence times in the binding site. There are many potential interactions if those factors are considered and reasonably well understood. In these terms, the identification of side-chain rotamer rearrangements upon ligand binding in combination with the use of the global RMSD comparison between two protein conformers is more informative. Thus, the incorporation of predictive tools of side-chain flexibility in protein/ligand interactions is key to infer dynamic aspects in molecular docking. Besides, the experimental evaluation of new drugs from this perspective becomes pivotal in the rational design of therapeutic strategies to control several physiological disorders and face emerging channelopathies.
Acknowledgments
The authors wish to thank the Division of Postgraduate Studies and Research (DEPI) of the Technological Center of Mexico, Veracruz campus, for the facilities for conducting this study.
Notes
FlexiProt 2.0 is a software designed for the prediction of flexibility profiles in primary sequences. Today, our group is working to share it in the public domain. For more information or in case of interest, contact the corresponding author at: daniel.bm@veracruz.tecnm.mx.
\n',keywords:"voltage sensor, side-chain flexibility, side-chain rotamers, RMSD, induced-fit docking, conformational selection",chapterPDFUrl:"https://cdn.intechopen.com/pdfs/80157.pdf",chapterXML:"https://mts.intechopen.com/source/xml/80157.xml",downloadPdfUrl:"/chapter/pdf-download/80157",previewPdfUrl:"/chapter/pdf-preview/80157",totalDownloads:100,totalViews:0,totalCrossrefCites:0,dateSubmitted:"December 12th 2021",dateReviewed:"December 20th 2021",datePrePublished:"January 21st 2022",datePublished:null,dateFinished:"January 21st 2022",readingETA:"0",abstract:"After ligand binding, many ion channels undergo rearrangements at the voltage sensor domain (VSD) that often modulate their gating activity with important physiological repercussions. Since the VSD is dynamic, it is interesting to establish a correlation between the potential mobility of this element in terms of its intrinsic flexibility and its ability to accommodate several ligands by induced-fit mechanisms. We presume that these associations are not causal since the flexibility of the VSD could have an important impact on the ligand coupling event. Many significantly flexible ion channels show a general architecture and composition compatible with important conformational changes and capable of accommodating chemically diverse agonists. In this contribution, the structural bases of this subtle and probably unexpected relationship between the VSD flexibility and its influence during the dynamic coupling of the ligand are exposed. Thus, given its physiological relevance, the study of ion channel malfunction can be associated with ligand accommodation events to the VSD, which could depend on its local flexibility. This could contribute to a better understanding of the molecular bases of a variety of physiological disorders. In consequence, considering these effects during the protein/ligand interaction could be determinant to the rational design of novel drugs.",reviewType:"peer-reviewed",bibtexUrl:"/chapter/bibtex/80157",risUrl:"/chapter/ris/80157",signatures:"Abigail García-Morales, Aylin López-Palestino and Daniel Balleza",book:{id:"10838",type:"book",title:"Ion Channels - From Basic Properties to Medical Treatment",subtitle:null,fullTitle:"Ion Channels - From Basic Properties to Medical Treatment",slug:null,publishedDate:null,bookSignature:"Ph.D. Zuzana Sevcikova Tomaskova",coverURL:"https://cdn.intechopen.com/books/images_new/10838.jpg",licenceType:"CC BY 3.0",editedByType:null,isbn:"978-1-80355-550-8",printIsbn:"978-1-80355-549-2",pdfIsbn:"978-1-80355-551-5",isAvailableForWebshopOrdering:!0,editors:[{id:"232970",title:"Ph.D.",name:"Zuzana",middleName:null,surname:"Sevcikova Tomaskova",slug:"zuzana-sevcikova-tomaskova",fullName:"Zuzana Sevcikova Tomaskova"}],productType:{id:"1",title:"Edited Volume",chapterContentType:"chapter",authoredCaption:"Edited by"}},authors:null,sections:[{id:"sec_1",title:"1. Introduction",level:"1"},{id:"sec_2",title:"2. The voltage sensor domain as a pharmacological target",level:"1"},{id:"sec_2_2",title:"2.1 Side-chain flexibility and ligand accommodation",level:"2"},{id:"sec_3_2",title:"2.2 Three cases of study: Kv7.2, TRPM8, TRPV1",level:"2"},{id:"sec_5",title:"3. Side-chain flexibility and the dynamic nature of protein-ligand interactions",level:"1"},{id:"sec_6",title:"4. Conclusions",level:"1"},{id:"sec_7",title:"Acknowledgments",level:"1"},{id:"sec_7",title:"Notes",level:"1"}],chapterReferences:[{id:"B1",body:'Balleza D, Quinto C, Elias D, Gómez-Lagunas F. A high-conductance cation channel from the inner membrane of the free-living soil bacteria Rhizobium etli. Archives of Microbiology. 2010;192(7):595-602. DOI: 10.1007/s00203-010-0587-3'},{id:"B2",body:'Labarca P, Bacigalupo J. Ion channels from chemosensory olfactory neurons. Journal of Bioenergetics and Biomembranes. 1988;20(5):551-569. 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Tecnológico Nacional De México/IT-Veracruz, Veracruz, Mexico
Tecnológico Nacional De México/IT-Veracruz, Veracruz, Mexico
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These metabolites are generated spontaneously by endogenous cellular processes and also by environmental agents. Because most of these lesions are promutagenic, linked to diverse disease-associated somatic mutations, as well as heritable single nucleotide polymorphisms (SNPs) in the normal human population, their prompt repair is warranted. Impairment of repair leading to mutation, a hallmark of cancer, underscores the essentiality of BER for maintaining genome integrity in humans and other mammals. In mammals, repair of oxidized bases and other BER substrates is initiated by DNA glycosylases (DGs), which excise the damaged bases and cleave the DNA strands at the resulting AP sites, followed by sequential end processing, gap-filling DNA synthesis, and ligation. In vitro BER performed with naked DNA substrates has been extensively studied, which delineates its basic mechanistic steps and subpathways. However, recent interest is directed to unraveling BER in cell chromatin, including its regulation via posttranslational modifications (PTMs), which occurs possibly in concert with nucleosome remodeling. Emerging reports on various PTMs of BER enzymes indicate that the PTMs, while dispensable for the enzymatic activity, regulate overall repair by modulating interactions with other repair proteins and chromatin factors, assembly of BER complexes, as well as turnover of the proteins, and may ultimately dictate the cellular phenotype. Here, we discuss recent advances in the BER field by reviewing the PTMs and how they regulate BER in chromatin.",signatures:"Shiladitya Sengupta, Chunying Yang, Bradley J. Eckelmann, Muralidhar L. 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He started his teaching career at Youjiang Medical University for Nationalities, Bose, in 2004. He obtained his PhD degree in Tumor Pathology at the Shanghai Jiao Tong University, Shanghai, China. His research focuses on the analysis of aflatoxin toxification and detection, hepatocellular carcinoma genetics, molecular mechanisms, epidemiology, and tumor susceptibility. His current research interests focus on the association between aflatoxins and hepatocarcinoma. He has more than 50 publications, serves on the editorial boards of seven journals, and regularly reviews for 25 journals and five granting bodies. 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Hegde",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/264616/images/system/264616.png",biography:"Dr. Hegde is Associate Professor at Houston Methodist Research Institute (HMRI), Houston, Texas, USA. He also holds adjunct faculty appointments at Weill Medical College of Cornell University and Texas A&M University. Dr. Hegde directs a research program focused on delineating the molecular insights into the involvement of genome damage/repair responses in human brain pathologies and developing novel mechanism-based treatment strategies for these diseases. Amyotrophic Lateral Sclerosis is a major focus of Dr. Hegde’s research program, with recent publications in prestigious journals that include Nature Communications, PNAS and JBC on this topic. Dr. Hegde’s research has been continuously funded by multiple grants from the National Institutes of Health and other foundations. 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Your Author Service Manager will inform you of any items not covered by the OAPF and provide exact information regarding those additional costs before proceeding.
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Open Access Funding
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To explore funding opportunities and learn more about how you can finance your IntechOpen publication, go to our Open Access Funding page. IntechOpen offers expert assistance to all of its Authors. We can support you in approaching funding bodies and institutions in relation to publishing fees by providing information about compliance with the Open Access policies of your funder or institution. We can also assist with communicating the benefits of Open Access in order to support and strengthen your funding request and provide personal guidance through your application process. You can contact us at funders@intechopen.com for further details or assistance.
\n\n
For Authors who are still unable to obtain funding from their institutions or research funding bodies for individual projects, IntechOpen does offer the possibility of applying for a Waiver to offset some or all processing feed. Details regarding our Waiver Policy can be found here.
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Added Value of Publishing with IntechOpen
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Choosing to publish with IntechOpen ensures the following benefits:
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Indexing and listing across major repositories, see details ...
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Long-term archiving
\n\t
Visibility on the world's strongest OA platform
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Live Performance Metrics to track readership and the impact of your chapter
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Dissemination and Promotion
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Benefits of Publishing with IntechOpen
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Proven world leader in Open Access book publishing with over 10 years experience
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Most competitive prices in the market
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The digitization of the urban environment, its building and infrastructural heritage and its services is at the center of the concept of smart city, and this appears strongly linked to the use of BIM on an increasingly extended scale as an enabling tool for planning cities that are increasingly intelligent, sustainable, interconnected and above all liveable. In this chapter a creation process for the digitalization of existing roads, as well-known as reverse engineering method, will be shown as follows: a) modeling 3D digital terrain model; b) creating the horizontal alignment, vertical profiles and editing cross-sections; c) modeling the 3D corridor. As a response to long-term development between BIM and road engineering, this chapter will contribute also by offering innovative and practical solutions for integration of road design and pavement analysis, for a better management and optimization of road pavement maintenance.",book:{id:"9872",slug:"models-and-technologies-for-smart-sustainable-and-safe-transportation-systems",title:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems",fullTitle:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems"},signatures:"Salvatore Antonio Biancardo, Nunzio Viscione, Cristina Oreto and Francesca Russo",authors:[{id:"300972",title:"Dr.",name:"Salvatore Antonio",middleName:null,surname:"Biancardo",slug:"salvatore-antonio-biancardo",fullName:"Salvatore Antonio Biancardo"},{id:"321425",title:"Prof.",name:"Francesca",middleName:null,surname:"Russo",slug:"francesca-russo",fullName:"Francesca Russo"},{id:"327976",title:"Mr.",name:"Nunzio",middleName:null,surname:"Viscione",slug:"nunzio-viscione",fullName:"Nunzio Viscione"},{id:"327977",title:"Ms.",name:"Cristina",middleName:null,surname:"Oreto",slug:"cristina-oreto",fullName:"Cristina Oreto"}]},{id:"64211",doi:"10.5772/intechopen.81159",title:"Contemporary Inspection and Monitoring for High-Speed Rail System",slug:"contemporary-inspection-and-monitoring-for-high-speed-rail-system",totalDownloads:1506,totalCrossrefCites:1,totalDimensionsCites:3,abstract:"Non-destructive testing (NDT) techniques have been explored and extensively utilised to help maintaining safety operation and improving ride comfort of the rail system. As an ascension of NDT techniques, the structural health monitoring (SHM) brings a new era of real-time condition assessment of rail system without interrupting train service, which is significantly meaningful to high-speed rail (HSR). This chapter first gives a review of NDT techniques of wheels and rails, followed by the recent applications of SHM on HSR enabled by a combination of advanced sensing technologies using optical fibre, piezoelectric and other smart sensors for on-board and online monitoring of the railway system from vehicles to rail infrastructure. An introduction of research frontier and development direction of SHM on HSR is provided subsequently concerning both sensing accuracy and efficiency, through cutting-edge data-driven analytic studies embracing such as wireless sensing and compressive sensing, which answer for the big data’s call brought by the new age of this transport.",book:{id:"7524",slug:"high-speed-rail",title:"High-Speed Rail",fullTitle:"High-Speed Rail"},signatures:"Lu Zhou, Xiao-Zhou Liu and Yi-Qing Ni",authors:[{id:"253578",title:"Dr.",name:"Lu",middleName:null,surname:"Zhou",slug:"lu-zhou",fullName:"Lu Zhou"},{id:"254448",title:"Prof.",name:"Yi-Qing",middleName:null,surname:"Ni",slug:"yi-qing-ni",fullName:"Yi-Qing Ni"},{id:"270970",title:"Dr.",name:"Xiao-Zhou",middleName:null,surname:"Liu",slug:"xiao-zhou-liu",fullName:"Xiao-Zhou Liu"}]},{id:"73356",doi:"10.5772/intechopen.93892",title:"Optimal Management of Electrified and Cooperative Bus Systems",slug:"optimal-management-of-electrified-and-cooperative-bus-systems",totalDownloads:353,totalCrossrefCites:1,totalDimensionsCites:1,abstract:"This chapter presents an integrated management approach exploiting the potentials of the new Cooperative Intelligent Transportation Systems (C-ITS) to meet the requirements of the next generation Public Transport (PT). This approach considers the additional complexity of electrification—for instance electric busses need to periodically recharge during operation using dedicated infrastructure. This not only can impact service level, but also extend operating costs with complex electric charges. We develop new strategies explicitly optimizing the interactions within the PT ecosystem consisting of vehicles, traffic signals, and e-bus charging infrastructure. To achieve these goals, we rely on vehicle control rather than on the use of transit signal priority, which in congested urban scenarios can have negative effects on overall traffic performance. The main research challenges are in formulating and solving complex multi-objective optimization problems and real-time control. The proposed system is tested and evaluated in simulation showing the benefits of electrified and cooperative bus systems.",book:{id:"9872",slug:"models-and-technologies-for-smart-sustainable-and-safe-transportation-systems",title:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems",fullTitle:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems"},signatures:"Francesco Viti, Marco Rinaldi and Georgios Laskaris",authors:[{id:"321907",title:"Dr.",name:"Francesco",middleName:null,surname:"Viti",slug:"francesco-viti",fullName:"Francesco Viti"},{id:"328609",title:"Dr.",name:"Marco",middleName:null,surname:"Rinaldi",slug:"marco-rinaldi",fullName:"Marco Rinaldi"},{id:"328610",title:"Dr.",name:"Georgios",middleName:null,surname:"Laskaris",slug:"georgios-laskaris",fullName:"Georgios Laskaris"}]},{id:"73821",doi:"10.5772/intechopen.94354",title:"Driver Assistance Technologies",slug:"driver-assistance-technologies",totalDownloads:600,totalCrossrefCites:0,totalDimensionsCites:1,abstract:"Topic: Driver Assistance Technology is emerging as new driving technology popularly known as ADAS. It is supported with Adaptive Cruise Control, Automatic Emergency Brake, blind spot monitoring, lane change assistance, and forward collision warnings etc. It is an important platform to integrate these multiple applications by using data from multifunction sensors, cameras, radars, lidars etc. and send command to plural actuators, engine, brake, steering etc. ADAS technology can detect some objects, do basic classification, alert the driver of hazardous road conditions, and in some cases, slow or stop the vehicle. The architecture of the electronic control units (ECUs) is responsible for executing advanced driver assistance systems (ADAS) in vehicle which is changing as per its response during the process of driving. Automotive system architecture integrates multiple applications into ADAS ECUs that serve multiple sensors for their functions. Hardware architecture of ADAS and autonomous driving, includes automotive Ethernet, TSN, Ethernet switch and gateway, and domain controller while Software architecture of ADAS and autonomous driving, including AUTOSAR Classic and Adaptive, ROS 2.0 and QNX. This chapter explains the functioning of Assistance Driving Technology with the help of its architecture and various types of sensors.",book:{id:"9872",slug:"models-and-technologies-for-smart-sustainable-and-safe-transportation-systems",title:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems",fullTitle:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems"},signatures:"Pradip Kumar Sarkar",authors:[{id:"321704",title:"Dr.",name:"Pradip Kumar",middleName:null,surname:"Sarkar",slug:"pradip-kumar-sarkar",fullName:"Pradip Kumar Sarkar"}]},{id:"63242",doi:"10.5772/intechopen.80302",title:"Main Ways to Improve Cutting Tools for Machine Wheel Tread Profile",slug:"main-ways-to-improve-cutting-tools-for-machine-wheel-tread-profile",totalDownloads:975,totalCrossrefCites:1,totalDimensionsCites:1,abstract:"This chapter considers the methods to increase the performance and reliability of the reprofile machining of the wheel tread profile. Proceeding from the fact that both in milling and turning, the cutting tool is a key element to ensure performance and reliability of the manufacturing process, the study considers the methods to increase the performance properties of cutting tools. In particular, the study includes the investigation of the following ways to improve cutting tools (carbide inserts) to machine wheel tread profile: replacement of traditional grades of WC-TiC-Co carbides with more efficient ones based on WC-TiC-TaC-Co; application of special thermally conductive pads, gaskets, and pastes to improve the distribution of heat flows in the cutting zone; and application of modern nanoscale composite multilayer coatings (NMCC). It is noted that even higher performance can be obtained by combining the above three methods, in particular, by combining application of special thermal pads and NMCC.",book:{id:"7524",slug:"high-speed-rail",title:"High-Speed Rail",fullTitle:"High-Speed Rail"},signatures:"Alexey Vereschaka, Popov Alexey, Grigoriev Sergey, Kulikov Mikhail and Sotova Catherine",authors:[{id:"196459",title:"Dr.",name:"Alexey",middleName:null,surname:"Vereschaka",slug:"alexey-vereschaka",fullName:"Alexey Vereschaka"},{id:"264332",title:"Dr.",name:"Alexey",middleName:null,surname:"Popov",slug:"alexey-popov",fullName:"Alexey Popov"},{id:"264333",title:"Prof.",name:"Sergey",middleName:null,surname:"Grigoriev",slug:"sergey-grigoriev",fullName:"Sergey Grigoriev"},{id:"264334",title:"Prof.",name:"Mikhail",middleName:null,surname:"Kulikov",slug:"mikhail-kulikov",fullName:"Mikhail Kulikov"},{id:"264336",title:"Dr.",name:"Catherine",middleName:null,surname:"Sotova",slug:"catherine-sotova",fullName:"Catherine Sotova"}]}],mostDownloadedChaptersLast30Days:[{id:"73624",title:"BIM Approach for Smart Infrastructure Design and Maintenance Operations",slug:"bim-approach-for-smart-infrastructure-design-and-maintenance-operations",totalDownloads:553,totalCrossrefCites:4,totalDimensionsCites:6,abstract:"In the age of the Internet-of-Things and Big Data, Building Information Modeling (BIM) is being expanded into sectors for which it was not originally designed, such as the infrastructure sector, and becomes a necessity for the planning and management of smart cities. The digitization of the urban environment, its building and infrastructural heritage and its services is at the center of the concept of smart city, and this appears strongly linked to the use of BIM on an increasingly extended scale as an enabling tool for planning cities that are increasingly intelligent, sustainable, interconnected and above all liveable. In this chapter a creation process for the digitalization of existing roads, as well-known as reverse engineering method, will be shown as follows: a) modeling 3D digital terrain model; b) creating the horizontal alignment, vertical profiles and editing cross-sections; c) modeling the 3D corridor. As a response to long-term development between BIM and road engineering, this chapter will contribute also by offering innovative and practical solutions for integration of road design and pavement analysis, for a better management and optimization of road pavement maintenance.",book:{id:"9872",slug:"models-and-technologies-for-smart-sustainable-and-safe-transportation-systems",title:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems",fullTitle:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems"},signatures:"Salvatore Antonio Biancardo, Nunzio Viscione, Cristina Oreto and Francesca Russo",authors:[{id:"300972",title:"Dr.",name:"Salvatore Antonio",middleName:null,surname:"Biancardo",slug:"salvatore-antonio-biancardo",fullName:"Salvatore Antonio Biancardo"},{id:"321425",title:"Prof.",name:"Francesca",middleName:null,surname:"Russo",slug:"francesca-russo",fullName:"Francesca Russo"},{id:"327976",title:"Mr.",name:"Nunzio",middleName:null,surname:"Viscione",slug:"nunzio-viscione",fullName:"Nunzio Viscione"},{id:"327977",title:"Ms.",name:"Cristina",middleName:null,surname:"Oreto",slug:"cristina-oreto",fullName:"Cristina Oreto"}]},{id:"73821",title:"Driver Assistance Technologies",slug:"driver-assistance-technologies",totalDownloads:600,totalCrossrefCites:0,totalDimensionsCites:1,abstract:"Topic: Driver Assistance Technology is emerging as new driving technology popularly known as ADAS. It is supported with Adaptive Cruise Control, Automatic Emergency Brake, blind spot monitoring, lane change assistance, and forward collision warnings etc. It is an important platform to integrate these multiple applications by using data from multifunction sensors, cameras, radars, lidars etc. and send command to plural actuators, engine, brake, steering etc. ADAS technology can detect some objects, do basic classification, alert the driver of hazardous road conditions, and in some cases, slow or stop the vehicle. The architecture of the electronic control units (ECUs) is responsible for executing advanced driver assistance systems (ADAS) in vehicle which is changing as per its response during the process of driving. Automotive system architecture integrates multiple applications into ADAS ECUs that serve multiple sensors for their functions. Hardware architecture of ADAS and autonomous driving, includes automotive Ethernet, TSN, Ethernet switch and gateway, and domain controller while Software architecture of ADAS and autonomous driving, including AUTOSAR Classic and Adaptive, ROS 2.0 and QNX. This chapter explains the functioning of Assistance Driving Technology with the help of its architecture and various types of sensors.",book:{id:"9872",slug:"models-and-technologies-for-smart-sustainable-and-safe-transportation-systems",title:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems",fullTitle:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems"},signatures:"Pradip Kumar Sarkar",authors:[{id:"321704",title:"Dr.",name:"Pradip Kumar",middleName:null,surname:"Sarkar",slug:"pradip-kumar-sarkar",fullName:"Pradip Kumar Sarkar"}]},{id:"63054",title:"Optimization of Components of Superstructure of High-Speed Rail: The Spanish Experience",slug:"optimization-of-components-of-superstructure-of-high-speed-rail-the-spanish-experience",totalDownloads:917,totalCrossrefCites:0,totalDimensionsCites:0,abstract:"The performance of rail transport has increased significantly in recent decades, in particular due to the gradual introduction of high-speed rails worldwide. In 1981, the first high-speed line of the world was inaugurated; nowadays, high-speed is operating in more than 20 countries, the high-speed network covering more than 35,000 kms (with more than 25,000 additional kms under construction). Spain is the second country by total distance of railways installed (only behind China) and the first in terms relative to the population and surface. Since the installation of the first high-speed line in Spain in 1992, the elements of the superstructure have undergone a continuous evolution, in order to improve the performance, the durability of the components and the comfort of the passengers. This evolution rests on an adequate selection of materials based on the characterization of their physical and mechanical properties to ensure the optimum in-service conditions. This chapter includes an overview of the different elements present in the railway superstructure of the high-speed lines in Spain. Throughout the text, the innovations incorporated over time are analyzed, as well as the methods used to validate them. In particular, a description of the mechanical characterization procedures is presented.",book:{id:"7524",slug:"high-speed-rail",title:"High-Speed Rail",fullTitle:"High-Speed Rail"},signatures:"Estela Ruiz, Isidro A. Carrascal, Diego Ferreño, José A. Casado and Soraya Diego",authors:[{id:"38018",title:"Prof.",name:"Diego",middleName:null,surname:"Ferreño",slug:"diego-ferreno",fullName:"Diego Ferreño"},{id:"264427",title:"Dr.",name:"Isidro A.",middleName:null,surname:"Carrascal",slug:"isidro-a.-carrascal",fullName:"Isidro A. Carrascal"},{id:"264428",title:"Prof.",name:"José A.",middleName:null,surname:"Casado",slug:"jose-a.-casado",fullName:"José A. Casado"},{id:"264429",title:"Dr.",name:"Soraya",middleName:null,surname:"Diego",slug:"soraya-diego",fullName:"Soraya Diego"},{id:"268961",title:"Dr.",name:"Estela",middleName:null,surname:"Ruiz",slug:"estela-ruiz",fullName:"Estela Ruiz"}]},{id:"63242",title:"Main Ways to Improve Cutting Tools for Machine Wheel Tread Profile",slug:"main-ways-to-improve-cutting-tools-for-machine-wheel-tread-profile",totalDownloads:975,totalCrossrefCites:1,totalDimensionsCites:1,abstract:"This chapter considers the methods to increase the performance and reliability of the reprofile machining of the wheel tread profile. Proceeding from the fact that both in milling and turning, the cutting tool is a key element to ensure performance and reliability of the manufacturing process, the study considers the methods to increase the performance properties of cutting tools. In particular, the study includes the investigation of the following ways to improve cutting tools (carbide inserts) to machine wheel tread profile: replacement of traditional grades of WC-TiC-Co carbides with more efficient ones based on WC-TiC-TaC-Co; application of special thermally conductive pads, gaskets, and pastes to improve the distribution of heat flows in the cutting zone; and application of modern nanoscale composite multilayer coatings (NMCC). It is noted that even higher performance can be obtained by combining the above three methods, in particular, by combining application of special thermal pads and NMCC.",book:{id:"7524",slug:"high-speed-rail",title:"High-Speed Rail",fullTitle:"High-Speed Rail"},signatures:"Alexey Vereschaka, Popov Alexey, Grigoriev Sergey, Kulikov Mikhail and Sotova Catherine",authors:[{id:"196459",title:"Dr.",name:"Alexey",middleName:null,surname:"Vereschaka",slug:"alexey-vereschaka",fullName:"Alexey Vereschaka"},{id:"264332",title:"Dr.",name:"Alexey",middleName:null,surname:"Popov",slug:"alexey-popov",fullName:"Alexey Popov"},{id:"264333",title:"Prof.",name:"Sergey",middleName:null,surname:"Grigoriev",slug:"sergey-grigoriev",fullName:"Sergey Grigoriev"},{id:"264334",title:"Prof.",name:"Mikhail",middleName:null,surname:"Kulikov",slug:"mikhail-kulikov",fullName:"Mikhail Kulikov"},{id:"264336",title:"Dr.",name:"Catherine",middleName:null,surname:"Sotova",slug:"catherine-sotova",fullName:"Catherine Sotova"}]},{id:"74333",title:"Transit Signal Priority in Smart Cities",slug:"transit-signal-priority-in-smart-cities",totalDownloads:447,totalCrossrefCites:0,totalDimensionsCites:0,abstract:"Giving priority to public transport vehicles at traffic signals is one of the traffic management strategies deployed at emerging smart cities to increase the quality of service for public transit users. It is a key to breaking the vicious cycle of congestion that threatens to bring cities into gridlock. In that cycle, increasing private traffic makes public transport become slower, less reliable, and less attractive. This results in deteriorated transit speed and reliability and induces more people to leave public transit in favor of the private cars, which create more traffic congestion, generate emissions, and increase energy consumption. Prioritizing public transit would break the vicious cycle and make it a more attractive mode as traffic demand and urban networks grow. A traditional way of protecting public transit from congestion is to move it either underground or above ground, as in the form of a metro/subway or air rail or create a dedicated lane as in the form of bus lane or light rail transit (LRT). However, due to the enormous capital expense involved or the lack of right-of-way, these solutions are often limited to few travel corridors or where money is not an issue. An alternative to prioritizing space to transit is to prioritize transit through time in the form of Transit Signal Priority (TSP). Noteworthy, transit and specifically bus schedules are known to be unstable and can be thrown off their schedule with even small changes in traffic or dwell time. At the same time, transit service reliability is an important factor for passengers and transit agencies. Less variability in transit travel time will need less slack or layover time. Thus, transit schedulers are interested in reducing transit travel time and its variability. One way to reach this goal is through an active intervention like TSP. In this chapter a comprehensive review of transit signal priority models is presented. The studies are classified into different categories which are: signal priority and different control systems, passive versus active priority, predictive transit signal priority, priority with connected vehicles, multi-modal signal priority models, and other practical considerations.",book:{id:"9872",slug:"models-and-technologies-for-smart-sustainable-and-safe-transportation-systems",title:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems",fullTitle:"Models and Technologies for Smart, Sustainable and Safe Transportation Systems"},signatures:"Bahman Moghimi and Camille Kamga",authors:[{id:"321370",title:"Dr.",name:"Bahman",middleName:null,surname:"Moghimi",slug:"bahman-moghimi",fullName:"Bahman Moghimi"},{id:"340958",title:"Prof.",name:"Camille",middleName:null,surname:"Kamga",slug:"camille-kamga",fullName:"Camille Kamga"}]}],onlineFirstChaptersFilter:{topicId:"713",limit:6,offset:0},onlineFirstChaptersCollection:[],onlineFirstChaptersTotal:0},preDownload:{success:null,errors:{}},subscriptionForm:{success:null,errors:{}},aboutIntechopen:{},privacyPolicy:{},peerReviewing:{},howOpenAccessPublishingWithIntechopenWorks:{},sponsorshipBooks:{sponsorshipBooks:[],offset:0,limit:8,total:null},allSeries:{pteSeriesList:[{id:"14",title:"Artificial Intelligence",numberOfPublishedBooks:9,numberOfPublishedChapters:89,numberOfOpenTopics:6,numberOfUpcomingTopics:0,issn:"2633-1403",doi:"10.5772/intechopen.79920",isOpenForSubmission:!0},{id:"7",title:"Biomedical Engineering",numberOfPublishedBooks:12,numberOfPublishedChapters:104,numberOfOpenTopics:3,numberOfUpcomingTopics:0,issn:"2631-5343",doi:"10.5772/intechopen.71985",isOpenForSubmission:!0}],lsSeriesList:[{id:"11",title:"Biochemistry",numberOfPublishedBooks:32,numberOfPublishedChapters:318,numberOfOpenTopics:4,numberOfUpcomingTopics:0,issn:"2632-0983",doi:"10.5772/intechopen.72877",isOpenForSubmission:!0},{id:"25",title:"Environmental Sciences",numberOfPublishedBooks:1,numberOfPublishedChapters:12,numberOfOpenTopics:4,numberOfUpcomingTopics:0,issn:"2754-6713",doi:"10.5772/intechopen.100362",isOpenForSubmission:!0},{id:"10",title:"Physiology",numberOfPublishedBooks:11,numberOfPublishedChapters:141,numberOfOpenTopics:4,numberOfUpcomingTopics:0,issn:"2631-8261",doi:"10.5772/intechopen.72796",isOpenForSubmission:!0}],hsSeriesList:[{id:"3",title:"Dentistry",numberOfPublishedBooks:8,numberOfPublishedChapters:129,numberOfOpenTopics:2,numberOfUpcomingTopics:0,issn:"2631-6218",doi:"10.5772/intechopen.71199",isOpenForSubmission:!0},{id:"6",title:"Infectious Diseases",numberOfPublishedBooks:13,numberOfPublishedChapters:113,numberOfOpenTopics:3,numberOfUpcomingTopics:1,issn:"2631-6188",doi:"10.5772/intechopen.71852",isOpenForSubmission:!0},{id:"13",title:"Veterinary Medicine and Science",numberOfPublishedBooks:11,numberOfPublishedChapters:106,numberOfOpenTopics:3,numberOfUpcomingTopics:0,issn:"2632-0517",doi:"10.5772/intechopen.73681",isOpenForSubmission:!0}],sshSeriesList:[{id:"22",title:"Business, Management and Economics",numberOfPublishedBooks:1,numberOfPublishedChapters:19,numberOfOpenTopics:2,numberOfUpcomingTopics:1,issn:"2753-894X",doi:"10.5772/intechopen.100359",isOpenForSubmission:!0},{id:"23",title:"Education and Human Development",numberOfPublishedBooks:0,numberOfPublishedChapters:5,numberOfOpenTopics:1,numberOfUpcomingTopics:1,issn:null,doi:"10.5772/intechopen.100360",isOpenForSubmission:!0},{id:"24",title:"Sustainable Development",numberOfPublishedBooks:0,numberOfPublishedChapters:15,numberOfOpenTopics:5,numberOfUpcomingTopics:0,issn:null,doi:"10.5772/intechopen.100361",isOpenForSubmission:!0}],testimonialsList:[{id:"6",text:"It is great to work with the IntechOpen to produce a worthwhile collection of research that also becomes a great educational resource and guide for future research endeavors.",author:{id:"259298",name:"Edward",surname:"Narayan",institutionString:null,profilePictureURL:"https://mts.intechopen.com/storage/users/259298/images/system/259298.jpeg",slug:"edward-narayan",institution:{id:"3",name:"University of Queensland",country:{id:null,name:"Australia"}}}},{id:"13",text:"The collaboration with and support of the technical staff of IntechOpen is fantastic. The whole process of submitting an article and editing of the submitted article goes extremely smooth and fast, the number of reads and downloads of chapters is high, and the contributions are also frequently cited.",author:{id:"55578",name:"Antonio",surname:"Jurado-Navas",institutionString:null,profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bRisIQAS/Profile_Picture_1626166543950",slug:"antonio-jurado-navas",institution:{id:"720",name:"University of Malaga",country:{id:null,name:"Spain"}}}}]},series:{item:{id:"14",title:"Artificial Intelligence",doi:"10.5772/intechopen.79920",issn:"2633-1403",scope:"Artificial Intelligence (AI) is a rapidly developing multidisciplinary research area that aims to solve increasingly complex problems. In today's highly integrated world, AI promises to become a robust and powerful means for obtaining solutions to previously unsolvable problems. This Series is intended for researchers and students alike interested in this fascinating field and its many applications.",coverUrl:"https://cdn.intechopen.com/series/covers/14.jpg",latestPublicationDate:"June 11th, 2022",hasOnlineFirst:!0,numberOfPublishedBooks:9,editor:{id:"218714",title:"Prof.",name:"Andries",middleName:null,surname:"Engelbrecht",slug:"andries-engelbrecht",fullName:"Andries Engelbrecht",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bRNR8QAO/Profile_Picture_1622640468300",biography:"Andries Engelbrecht received the Masters and PhD degrees in Computer Science from the University of Stellenbosch, South Africa, in 1994 and 1999 respectively. He is currently appointed as the Voigt Chair in Data Science in the Department of Industrial Engineering, with a joint appointment as Professor in the Computer Science Division, Stellenbosch University. Prior to his appointment at Stellenbosch University, he has been at the University of Pretoria, Department of Computer Science (1998-2018), where he was appointed as South Africa Research Chair in Artifical Intelligence (2007-2018), the head of the Department of Computer Science (2008-2017), and Director of the Institute for Big Data and Data Science (2017-2018). In addition to a number of research articles, he has written two books, Computational Intelligence: An Introduction and Fundamentals of Computational Swarm Intelligence.",institutionString:null,institution:{name:"Stellenbosch University",institutionURL:null,country:{name:"South Africa"}}},editorTwo:null,editorThree:null},subseries:{paginationCount:6,paginationItems:[{id:"22",title:"Applied Intelligence",coverUrl:"https://cdn.intechopen.com/series_topics/covers/22.jpg",isOpenForSubmission:!0,editor:{id:"27170",title:"Prof.",name:"Carlos",middleName:"M.",surname:"Travieso-Gonzalez",slug:"carlos-travieso-gonzalez",fullName:"Carlos Travieso-Gonzalez",profilePictureURL:"https://mts.intechopen.com/storage/users/27170/images/system/27170.jpeg",biography:"Carlos M. Travieso-González received his MSc degree in Telecommunication Engineering at Polytechnic University of Catalonia (UPC), Spain in 1997, and his Ph.D. degree in 2002 at the University of Las Palmas de Gran Canaria (ULPGC-Spain). He is a full professor of signal processing and pattern recognition and is head of the Signals and Communications Department at ULPGC, teaching from 2001 on subjects on signal processing and learning theory. His research lines are biometrics, biomedical signals and images, data mining, classification system, signal and image processing, machine learning, and environmental intelligence. He has researched in 52 international and Spanish research projects, some of them as head researcher. He is co-author of 4 books, co-editor of 27 proceedings books, guest editor for 8 JCR-ISI international journals, and up to 24 book chapters. He has over 450 papers published in international journals and conferences (81 of them indexed on JCR – ISI - Web of Science). He has published seven patents in the Spanish Patent and Trademark Office. He has been a supervisor on 8 Ph.D. theses (11 more are under supervision), and 130 master theses. He is the founder of The IEEE IWOBI conference series and the president of its Steering Committee, as well as the founder of both the InnoEducaTIC and APPIS conference series. He is an evaluator of project proposals for the European Union (H2020), Medical Research Council (MRC, UK), Spanish Government (ANECA, Spain), Research National Agency (ANR, France), DAAD (Germany), Argentinian Government, and the Colombian Institutions. He has been a reviewer in different indexed international journals (<70) and conferences (<250) since 2001. He has been a member of the IASTED Technical Committee on Image Processing from 2007 and a member of the IASTED Technical Committee on Artificial Intelligence and Expert Systems from 2011. \n\nHe has held the general chair position for the following: ACM-APPIS (2020, 2021), IEEE-IWOBI (2019, 2020 and 2020), A PPIS (2018, 2019), IEEE-IWOBI (2014, 2015, 2017, 2018), InnoEducaTIC (2014, 2017), IEEE-INES (2013), NoLISP (2011), JRBP (2012), and IEEE-ICCST (2005)\n\nHe is an associate editor of the Computational Intelligence and Neuroscience Journal (Hindawi – Q2 JCR-ISI). He was vice dean from 2004 to 2010 in the Higher Technical School of Telecommunication Engineers at ULPGC and the vice dean of Graduate and Postgraduate Studies from March 2013 to November 2017. He won the “Catedra Telefonica” Awards in Modality of Knowledge Transfer, 2017, 2018, and 2019 editions, and awards in Modality of COVID Research in 2020.\n\nPublic References:\nResearcher ID http://www.researcherid.com/rid/N-5967-2014\nORCID https://orcid.org/0000-0002-4621-2768 \nScopus Author ID https://www.scopus.com/authid/detail.uri?authorId=6602376272\nScholar Google https://scholar.google.es/citations?user=G1ks9nIAAAAJ&hl=en \nResearchGate https://www.researchgate.net/profile/Carlos_Travieso",institutionString:null,institution:{name:"University of Las Palmas de Gran Canaria",institutionURL:null,country:{name:"Spain"}}},editorTwo:null,editorThree:null},{id:"23",title:"Computational Neuroscience",coverUrl:"https://cdn.intechopen.com/series_topics/covers/23.jpg",isOpenForSubmission:!0,editor:{id:"14004",title:"Dr.",name:"Magnus",middleName:null,surname:"Johnsson",slug:"magnus-johnsson",fullName:"Magnus Johnsson",profilePictureURL:"https://mts.intechopen.com/storage/users/14004/images/system/14004.png",biography:"Dr Magnus Johnsson is a cross-disciplinary scientist, lecturer, scientific editor and AI/machine learning consultant from Sweden. \n\nHe is currently at Malmö University in Sweden, but also held positions at Lund University in Sweden and at Moscow Engineering Physics Institute. \nHe holds editorial positions at several international scientific journals and has served as a scientific editor for books and special journal issues. \nHis research interests are wide and include, but are not limited to, autonomous systems, computer modeling, artificial neural networks, artificial intelligence, cognitive neuroscience, cognitive robotics, cognitive architectures, cognitive aids and the philosophy of mind. \n\nDr. Johnsson has experience from working in the industry and he has a keen interest in the application of neural networks and artificial intelligence to fields like industry, finance, and medicine. \n\nWeb page: www.magnusjohnsson.se",institutionString:null,institution:{name:"Malmö University",institutionURL:null,country:{name:"Sweden"}}},editorTwo:null,editorThree:null},{id:"24",title:"Computer Vision",coverUrl:"https://cdn.intechopen.com/series_topics/covers/24.jpg",isOpenForSubmission:!0,editor:{id:"294154",title:"Prof.",name:"George",middleName:null,surname:"Papakostas",slug:"george-papakostas",fullName:"George Papakostas",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002hYaGbQAK/Profile_Picture_1624519712088",biography:"George A. Papakostas has received a diploma in Electrical and Computer Engineering in 1999 and the M.Sc. and Ph.D. degrees in Electrical and Computer Engineering in 2002 and 2007, respectively, from the Democritus University of Thrace (DUTH), Greece. Dr. Papakostas serves as a Tenured Full Professor at the Department of Computer Science, International Hellenic University, Greece. Dr. Papakostas has 10 years of experience in large-scale systems design as a senior software engineer and technical manager, and 20 years of research experience in the field of Artificial Intelligence. Currently, he is the Head of the “Visual Computing” division of HUman-MAchines INteraction Laboratory (HUMAIN-Lab) and the Director of the MPhil program “Advanced Technologies in Informatics and Computers” hosted by the Department of Computer Science, International Hellenic University. He has (co)authored more than 150 publications in indexed journals, international conferences and book chapters, 1 book (in Greek), 3 edited books, and 5 journal special issues. His publications have more than 2100 citations with h-index 27 (GoogleScholar). His research interests include computer/machine vision, machine learning, pattern recognition, computational intelligence. \nDr. Papakostas served as a reviewer in numerous journals, as a program\ncommittee member in international conferences and he is a member of the IAENG, MIR Labs, EUCogIII, INSTICC and the Technical Chamber of Greece (TEE).",institutionString:null,institution:{name:"International Hellenic University",institutionURL:null,country:{name:"Greece"}}},editorTwo:null,editorThree:null},{id:"25",title:"Evolutionary Computation",coverUrl:"https://cdn.intechopen.com/series_topics/covers/25.jpg",isOpenForSubmission:!0,editor:{id:"136112",title:"Dr.",name:"Sebastian",middleName:null,surname:"Ventura Soto",slug:"sebastian-ventura-soto",fullName:"Sebastian Ventura Soto",profilePictureURL:"https://mts.intechopen.com/storage/users/136112/images/system/136112.png",biography:"Sebastian Ventura is a Spanish researcher, a full professor with the Department of Computer Science and Numerical Analysis, University of Córdoba. Dr Ventura also holds the positions of Affiliated Professor at Virginia Commonwealth University (Richmond, USA) and Distinguished Adjunct Professor at King Abdulaziz University (Jeddah, Saudi Arabia). Additionally, he is deputy director of the Andalusian Research Institute in Data Science and Computational Intelligence (DaSCI) and heads the Knowledge Discovery and Intelligent Systems Research Laboratory. He has published more than ten books and over 300 articles in journals and scientific conferences. Currently, his work has received over 18,000 citations according to Google Scholar, including more than 2200 citations in 2020. In the last five years, he has published more than 60 papers in international journals indexed in the JCR (around 70% of them belonging to first quartile journals) and he has edited some Springer books “Supervised Descriptive Pattern Mining” (2018), “Multiple Instance Learning - Foundations and Algorithms” (2016), and “Pattern Mining with Evolutionary Algorithms” (2016). He has also been involved in more than 20 research projects supported by the Spanish and Andalusian governments and the European Union. He currently belongs to the editorial board of PeerJ Computer Science, Information Fusion and Engineering Applications of Artificial Intelligence journals, being also associate editor of Applied Computational Intelligence and Soft Computing and IEEE Transactions on Cybernetics. Finally, he is editor-in-chief of Progress in Artificial Intelligence. He is a Senior Member of the IEEE Computer, the IEEE Computational Intelligence, and the IEEE Systems, Man, and Cybernetics Societies, and the Association of Computing Machinery (ACM). Finally, his main research interests include data science, computational intelligence, and their applications.",institutionString:null,institution:{name:"University of Córdoba",institutionURL:null,country:{name:"Spain"}}},editorTwo:null,editorThree:null},{id:"26",title:"Machine Learning and Data Mining",coverUrl:"https://cdn.intechopen.com/series_topics/covers/26.jpg",isOpenForSubmission:!0,editor:{id:"24555",title:"Dr.",name:"Marco Antonio",middleName:null,surname:"Aceves Fernandez",slug:"marco-antonio-aceves-fernandez",fullName:"Marco Antonio Aceves Fernandez",profilePictureURL:"https://mts.intechopen.com/storage/users/24555/images/system/24555.jpg",biography:"Dr. Marco Antonio Aceves Fernandez obtained his B.Sc. (Eng.) in Telematics from the Universidad de Colima, Mexico. He obtained both his M.Sc. and Ph.D. from the University of Liverpool, England, in the field of Intelligent Systems. He is a full professor at the Universidad Autonoma de Queretaro, Mexico, and a member of the National System of Researchers (SNI) since 2009. Dr. Aceves Fernandez has published more than 80 research papers as well as a number of book chapters and congress papers. He has contributed in more than 20 funded research projects, both academic and industrial, in the area of artificial intelligence, ranging from environmental, biomedical, automotive, aviation, consumer, and robotics to other applications. He is also a honorary president at the National Association of Embedded Systems (AMESE), a senior member of the IEEE, and a board member of many institutions. His research interests include intelligent and embedded systems.",institutionString:"Universidad Autonoma de Queretaro",institution:{name:"Autonomous University of Queretaro",institutionURL:null,country:{name:"Mexico"}}},editorTwo:null,editorThree:null},{id:"27",title:"Multi-Agent Systems",coverUrl:"https://cdn.intechopen.com/series_topics/covers/27.jpg",isOpenForSubmission:!0,editor:{id:"148497",title:"Dr.",name:"Mehmet",middleName:"Emin",surname:"Aydin",slug:"mehmet-aydin",fullName:"Mehmet Aydin",profilePictureURL:"https://mts.intechopen.com/storage/users/148497/images/system/148497.jpg",biography:"Dr. Mehmet Emin Aydin is a Senior Lecturer with the Department of Computer Science and Creative Technology, the University of the West of England, Bristol, UK. His research interests include swarm intelligence, parallel and distributed metaheuristics, machine learning, intelligent agents and multi-agent systems, resource planning, scheduling and optimization, combinatorial optimization. Dr. Aydin is currently a Fellow of Higher Education Academy, UK, a member of EPSRC College, a senior member of IEEE and a senior member of ACM. In addition to being a member of advisory committees of many international conferences, he is an Editorial Board Member of various peer-reviewed international journals. He has served as guest editor for a number of special issues of peer-reviewed international journals.",institutionString:null,institution:{name:"University of the West of England",institutionURL:null,country:{name:"United Kingdom"}}},editorTwo:null,editorThree:null}]},overviewPageOFChapters:{paginationCount:19,paginationItems:[{id:"82196",title:"Multi-Features Assisted Age Invariant Face Recognition and Retrieval Using CNN with Scale Invariant Heat Kernel Signature",doi:"10.5772/intechopen.104944",signatures:"Kamarajugadda Kishore Kumar and Movva Pavani",slug:"multi-features-assisted-age-invariant-face-recognition-and-retrieval-using-cnn-with-scale-invariant-",totalDownloads:6,totalCrossrefCites:0,totalDimensionsCites:0,authors:null,book:{title:"Pattern Recognition - New Insights",coverURL:"https://cdn.intechopen.com/books/images_new/11442.jpg",subseries:{id:"26",title:"Machine Learning and Data Mining"}}},{id:"82063",title:"Evaluating Similarities and Differences between Machine Learning and Traditional Statistical Modeling in Healthcare Analytics",doi:"10.5772/intechopen.105116",signatures:"Michele Bennett, Ewa J. 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Rodriguez-Morales",hash:"61c627da05b2ace83056d11357bdf361",volumeInSeries:3,fullTitle:"Current Topics in Neglected Tropical Diseases",editors:[{id:"131400",title:"Prof.",name:"Alfonso J.",middleName:null,surname:"Rodriguez-Morales",slug:"alfonso-j.-rodriguez-morales",fullName:"Alfonso J. Rodriguez-Morales",profilePictureURL:"https://mts.intechopen.com/storage/users/131400/images/system/131400.png",institutionString:"Institución Universitaria Visión de las Américas, Colombia",institution:null}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null},{type:"book",id:"7064",title:"Current Perspectives in Human Papillomavirus",subtitle:null,coverURL:"https://cdn.intechopen.com/books/images_new/7064.jpg",slug:"current-perspectives-in-human-papillomavirus",publishedDate:"May 2nd 2019",editedByType:"Edited by",bookSignature:"Shailendra K. 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Saxena",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bRET3QAO/Profile_Picture_2022-05-10T10:10:26.jpeg",institutionString:"King George's Medical University",institution:{name:"King George's Medical University",institutionURL:null,country:{name:"India"}}}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null}]},subseriesFiltersForPublishedBooks:[{group:"subseries",caption:"Bacterial Infectious Diseases",value:3,count:2},{group:"subseries",caption:"Parasitic Infectious Diseases",value:5,count:4},{group:"subseries",caption:"Viral Infectious Diseases",value:6,count:7}],publicationYearFilters:[{group:"publicationYear",caption:"2022",value:2022,count:2},{group:"publicationYear",caption:"2021",value:2021,count:4},{group:"publicationYear",caption:"2020",value:2020,count:3},{group:"publicationYear",caption:"2019",value:2019,count:3},{group:"publicationYear",caption:"2018",value:2018,count:1}],authors:{paginationCount:301,paginationItems:[{id:"116250",title:"Dr.",name:"Nima",middleName:null,surname:"Rezaei",slug:"nima-rezaei",fullName:"Nima Rezaei",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/116250/images/system/116250.jpg",biography:"Professor Nima Rezaei obtained an MD from Tehran University of Medical Sciences, Iran. He also obtained an MSc in Molecular and Genetic Medicine, and a Ph.D. in Clinical Immunology and Human Genetics from the University of Sheffield, UK. He also completed a short-term fellowship in Pediatric Clinical Immunology and Bone Marrow Transplantation at Newcastle General Hospital, England. Dr. Rezaei is a Full Professor of Immunology and Vice Dean of International Affairs and Research, at the School of Medicine, Tehran University of Medical Sciences, and the co-founder and head of the Research Center for Immunodeficiencies. He is also the founding president of the Universal Scientific Education and Research Network (USERN). Dr. Rezaei has directed more than 100 research projects and has designed and participated in several international collaborative projects. He is an editor, editorial assistant, or editorial board member of more than forty international journals. He has edited more than 50 international books, presented more than 500 lectures/posters in congresses/meetings, and published more than 1,100 scientific papers in international journals.",institutionString:"Tehran University of Medical Sciences",institution:{name:"Tehran University of Medical Sciences",country:{name:"Iran"}}},{id:"180733",title:"Dr.",name:"Jean",middleName:null,surname:"Engohang-Ndong",slug:"jean-engohang-ndong",fullName:"Jean Engohang-Ndong",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/180733/images/system/180733.png",biography:"Dr. Jean Engohang-Ndong was born and raised in Gabon. After obtaining his Associate Degree of Science at the University of Science and Technology of Masuku, Gabon, he continued his education in France where he obtained his BS, MS, and Ph.D. in Medical Microbiology. He worked as a post-doctoral fellow at the Public Health Research Institute (PHRI), Newark, NJ for four years before accepting a three-year faculty position at Brigham Young University-Hawaii. Dr. Engohang-Ndong is a tenured faculty member with the academic rank of Full Professor at Kent State University, Ohio, where he teaches a wide range of biological science courses and pursues his research in medical and environmental microbiology. Recently, he expanded his research interest to epidemiology and biostatistics of chronic diseases in Gabon.",institutionString:"Kent State University",institution:{name:"Kent State University",country:{name:"United States of America"}}},{id:"188773",title:"Prof.",name:"Emmanuel",middleName:null,surname:"Drouet",slug:"emmanuel-drouet",fullName:"Emmanuel Drouet",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/188773/images/system/188773.png",biography:"Emmanuel Drouet, PharmD, is a Professor of Virology at the Faculty of Pharmacy, the University Grenoble-Alpes, France. As a head scientist at the Institute of Structural Biology in Grenoble, Dr. Drouet’s research investigates persisting viruses in humans (RNA and DNA viruses) and the balance with our host immune system. He focuses on these viruses’ effects on humans (both their impact on pathology and their symbiotic relationships in humans). He has an excellent track record in the herpesvirus field, and his group is engaged in clinical research in the field of Epstein-Barr virus diseases. He is the editor of the online Encyclopedia of Environment and he coordinates the Universal Health Coverage education program for the BioHealth Computing Schools of the European Institute of Science.",institutionString:null,institution:{name:"Grenoble Alpes University",country:{name:"France"}}},{id:"131400",title:"Prof.",name:"Alfonso J.",middleName:null,surname:"Rodriguez-Morales",slug:"alfonso-j.-rodriguez-morales",fullName:"Alfonso J. Rodriguez-Morales",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/131400/images/system/131400.png",biography:"Dr. Rodriguez-Morales is an expert in tropical and emerging diseases, particularly zoonotic and vector-borne diseases (especially arboviral diseases). He is the president of the Travel Medicine Committee of the Pan-American Infectious Diseases Association (API), as well as the president of the Colombian Association of Infectious Diseases (ACIN). He is a member of the Committee on Tropical Medicine, Zoonoses, and Travel Medicine of ACIN. He is a vice-president of the Latin American Society for Travel Medicine (SLAMVI) and a Member of the Council of the International Society for Infectious Diseases (ISID). Since 2014, he has been recognized as a Senior Researcher, at the Ministry of Science of Colombia. He is a professor at the Faculty of Medicine of the Fundacion Universitaria Autonoma de las Americas, in Pereira, Risaralda, Colombia. He is an External Professor, Master in Research on Tropical Medicine and International Health, Universitat de Barcelona, Spain. He is also a professor at the Master in Clinical Epidemiology and Biostatistics, Universidad Científica del Sur, Lima, Peru. In 2021 he has been awarded the “Raul Isturiz Award” Medal of the API. Also, in 2021, he was awarded with the “Jose Felix Patiño” Asclepius Staff Medal of the Colombian Medical College, due to his scientific contributions to COVID-19 during the pandemic. He is currently the Editor in Chief of the journal Travel Medicine and Infectious Diseases. His Scopus H index is 47 (Google Scholar H index, 68).",institutionString:"Institución Universitaria Visión de las Américas, Colombia",institution:null},{id:"332819",title:"Dr.",name:"Chukwudi Michael",middleName:"Michael",surname:"Egbuche",slug:"chukwudi-michael-egbuche",fullName:"Chukwudi Michael Egbuche",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/332819/images/14624_n.jpg",biography:"I an Dr. Chukwudi Michael Egbuche. I am a Senior Lecturer in the Department of Parasitology and Entomology, Nnamdi Azikiwe University, Awka.",institutionString:null,institution:{name:"Nnamdi Azikiwe University",country:{name:"Nigeria"}}},{id:"284232",title:"Mr.",name:"Nikunj",middleName:"U",surname:"Tandel",slug:"nikunj-tandel",fullName:"Nikunj Tandel",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/284232/images/8275_n.jpg",biography:'Mr. Nikunj Tandel has completed his Master\'s degree in Biotechnology from VIT University, India in the year of 2012. He is having 8 years of research experience especially in the field of malaria epidemiology, immunology, and nanoparticle-based drug delivery system against the infectious diseases, autoimmune disorders and cancer. He has worked for the NIH funded-International Center of Excellence in Malaria Research project "Center for the study of complex malaria in India (CSCMi)" in collaboration with New York University. The preliminary objectives of the study are to understand and develop the evidence-based tools and interventions for the control and prevention of malaria in different sites of the INDIA. Alongside, with the help of next-generation genomics study, the team has studied the antimalarial drug resistance in India. Further, he has extended his research in the development of Humanized mice for the study of liver-stage malaria and identification of molecular marker(s) for the Artemisinin resistance. At present, his research focuses on understanding the role of B cells in the activation of CD8+ T cells in malaria. Received the CSIR-SRF (Senior Research Fellow) award-2018, FIMSA (Federation of Immunological Societies of Asia-Oceania) Travel Bursary award to attend the IUIS-IIS-FIMSA Immunology course-2019',institutionString:"Nirma University",institution:{name:"Nirma University",country:{name:"India"}}},{id:"334383",title:"Ph.D.",name:"Simone",middleName:"Ulrich",surname:"Ulrich Picoli",slug:"simone-ulrich-picoli",fullName:"Simone Ulrich Picoli",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/334383/images/15919_n.jpg",biography:"Graduated in Pharmacy from Universidade Luterana do Brasil (1999), Master in Agricultural and Environmental Microbiology from Federal University of Rio Grande do Sul (2002), Specialization in Clinical Microbiology from Universidade de São Paulo, USP (2007) and PhD in Sciences in Gastroenterology and Hepatology (2012). She is currently an Adjunct Professor at Feevale University in Medicine and Biomedicine courses and a permanent professor of the Academic Master\\'s Degree in Virology. She has experience in the field of Microbiology, with an emphasis on Bacteriology, working mainly on the following topics: bacteriophages, bacterial resistance, clinical microbiology and food microbiology.",institutionString:null,institution:{name:"Universidade Feevale",country:{name:"Brazil"}}},{id:"229220",title:"Dr.",name:"Amjad",middleName:"Islam",surname:"Aqib",slug:"amjad-aqib",fullName:"Amjad Aqib",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/229220/images/system/229220.png",biography:"Dr. Amjad Islam Aqib obtained a DVM and MSc (Hons) from University of Agriculture Faisalabad (UAF), Pakistan, and a PhD from the University of Veterinary and Animal Sciences Lahore, Pakistan. Dr. Aqib joined the Department of Clinical Medicine and Surgery at UAF for one year as an assistant professor where he developed a research laboratory designated for pathogenic bacteria. Since 2018, he has been Assistant Professor/Officer in-charge, Department of Medicine, Manager Research Operations and Development-ORIC, and President One Health Club at Cholistan University of Veterinary and Animal Sciences, Bahawalpur, Pakistan. He has nearly 100 publications to his credit. His research interests include epidemiological patterns and molecular analysis of antimicrobial resistance and modulation and vaccine development against animal pathogens of public health concern.",institutionString:"Cholistan University of Veterinary and Animal Sciences",institution:null},{id:"62900",title:"Prof.",name:"Fethi",middleName:null,surname:"Derbel",slug:"fethi-derbel",fullName:"Fethi Derbel",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/62900/images/system/62900.jpeg",biography:"Professor Fethi Derbel was born in 1960 in Tunisia. He received his medical degree from the Sousse Faculty of Medicine at Sousse, University of Sousse, Tunisia. He completed his surgical residency in General Surgery at the University Hospital Farhat Hached of Sousse and was a member of the Unit of Liver Transplantation in the University of Rennes, France. He then worked in the Department of Surgery at the Sahloul University Hospital in Sousse. Professor Derbel is presently working at the Clinique les Oliviers, Sousse, Tunisia. His hospital activities are mostly concerned with laparoscopic, colorectal, pancreatic, hepatobiliary, and gastric surgery. He is also very interested in hernia surgery and performs ventral hernia repairs and inguinal hernia repairs. He has been a member of the GREPA and Tunisian Hernia Society (THS). During his residency, he managed patients suffering from diabetic foot, and he was very interested in this pathology. For this reason, he decided to coordinate a book project dealing with the diabetic foot. Professor Derbel has published many articles in journals and collaborates intensively with IntechOpen Access Publisher as an editor.",institutionString:"Clinique les Oliviers",institution:null},{id:"300144",title:"Dr.",name:"Meriem",middleName:null,surname:"Braiki",slug:"meriem-braiki",fullName:"Meriem Braiki",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/300144/images/system/300144.jpg",biography:"Dr. Meriem Braiki is a specialist in pediatric surgeon from Tunisia. She was born in 1985. She received her medical degree from the University of Medicine at Sousse, Tunisia. She achieved her surgical residency training periods in Pediatric Surgery departments at University Hospitals in Monastir, Tunis and France.\r\nShe is currently working at the Pediatric surgery department, Sidi Bouzid Hospital, Tunisia. Her hospital activities are mostly concerned with laparoscopic, parietal, urological and digestive surgery. She has published several articles in diffrent journals.",institutionString:"Sidi Bouzid Regional Hospital",institution:null},{id:"229481",title:"Dr.",name:"Erika M.",middleName:"Martins",surname:"de Carvalho",slug:"erika-m.-de-carvalho",fullName:"Erika M. de Carvalho",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/229481/images/6397_n.jpg",biography:null,institutionString:null,institution:{name:"Oswaldo Cruz Foundation",country:{name:"Brazil"}}},{id:"186537",title:"Prof.",name:"Tonay",middleName:null,surname:"Inceboz",slug:"tonay-inceboz",fullName:"Tonay Inceboz",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/186537/images/system/186537.jfif",biography:"I was graduated from Ege University of Medical Faculty (Turkey) in 1988 and completed his Med. PhD degree in Medical Parasitology at the same university. I became an Associate Professor in 2008 and Professor in 2014. I am currently working as a Professor at the Department of Medical Parasitology at Dokuz Eylul University, Izmir, Turkey.\n\nI have given many lectures, presentations in different academic meetings. I have more than 60 articles in peer-reviewed journals, 18 book chapters, 1 book editorship.\n\nMy research interests are Echinococcus granulosus, Echinococcus multilocularis (diagnosis, life cycle, in vitro and in vivo cultivation), and Trichomonas vaginalis (diagnosis, PCR, and in vitro cultivation).",institutionString:"Dokuz Eylül University",institution:{name:"Dokuz Eylül University",country:{name:"Turkey"}}},{id:"71812",title:"Prof.",name:"Hanem Fathy",middleName:"Fathy",surname:"Khater",slug:"hanem-fathy-khater",fullName:"Hanem Fathy Khater",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/71812/images/1167_n.jpg",biography:"Prof. Khater is a Professor of Parasitology at Benha University, Egypt. She studied for her doctoral degree, at the Department of Entomology, College of Agriculture, Food and Natural Resources, University of Missouri, Columbia, USA. She has completed her Ph.D. degrees in Parasitology in Egypt, from where she got the award for “the best scientific Ph.D. dissertation”. She worked at the School of Biological Sciences, Bristol, England, the UK in controlling insects of medical and veterinary importance as a grant from Newton Mosharafa, the British Council. Her research is focused on searching of pesticides against mosquitoes, house flies, lice, green bottle fly, camel nasal botfly, soft and hard ticks, mites, and the diamondback moth as well as control of several parasites using safe and natural materials to avoid drug resistances and environmental contamination.",institutionString:null,institution:{name:"Banha University",country:{name:"Egypt"}}},{id:"99780",title:"Prof.",name:"Omolade",middleName:"Olayinka",surname:"Okwa",slug:"omolade-okwa",fullName:"Omolade Okwa",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/99780/images/system/99780.jpg",biography:"Omolade Olayinka Okwa is presently a Professor of Parasitology at Lagos State University, Nigeria. She has a PhD in Parasitology (1997), an MSc in Cellular Parasitology (1992), and a BSc (Hons) Zoology (1990) all from the University of Ibadan, Nigeria. She teaches parasitology at the undergraduate and postgraduate levels. She was a recipient of a Commonwealth fellowship supported by British Council tenable at the Centre for Entomology and Parasitology (CAEP), Keele University, United Kingdom between 2004 and 2005. She was awarded an Honorary Visiting Research Fellow at the same university from 2005 to 2007. \nShe has been an external examiner to the Department of Veterinary Microbiology and Parasitology, University of Ibadan, MSc programme between 2010 and 2012. She is a member of the Nigerian Society of Experimental Biology (NISEB), Parasitology and Public Health Society of Nigeria (PPSN), Science Association of Nigeria (SAN), Zoological Society of Nigeria (ZSN), and is Vice Chairperson of the Organisation of Women in Science (OWSG), LASU chapter. She served as Head of Department of Zoology and Environmental Biology, Lagos State University from 2007 to 2010 and 2014 to 2016. She is a reviewer for several local and international journals such as Unilag Journal of Science, Libyan Journal of Medicine, Journal of Medicine and Medical Sciences, and Annual Research and Review in Science. \nShe has authored 45 scientific research publications in local and international journals, 8 scientific reviews, 4 books, and 3 book chapters, which includes the books “Malaria Parasites” and “Malaria” which are IntechOpen access publications.",institutionString:"Lagos State University",institution:{name:"Lagos State University",country:{name:"Nigeria"}}},{id:"273100",title:"Dr.",name:"Vijay",middleName:null,surname:"Gayam",slug:"vijay-gayam",fullName:"Vijay Gayam",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/273100/images/system/273100.jpeg",biography:"Dr. Vijay Bhaskar Reddy Gayam is currently practicing as an internist at Interfaith Medical Center in Brooklyn, New York, USA. He is also a Clinical Assistant Professor at the SUNY Downstate University Hospital and Adjunct Professor of Medicine at the American University of Antigua. He is a holder of an M.B.B.S. degree bestowed to him by Osmania Medical College and received his M.D. at Interfaith Medical Center. His career goals thus far have heavily focused on direct patient care, medical education, and clinical research. He currently serves in two leadership capacities; Assistant Program Director of Medicine at Interfaith Medical Center and as a Councilor for the American\r\nFederation for Medical Research. As a true academician and researcher, he has more than 50 papers indexed in international peer-reviewed journals. He has also presented numerous papers in multiple national and international scientific conferences. His areas of research interest include general internal medicine, gastroenterology and hepatology. He serves as an editor, editorial board member and reviewer for multiple international journals. His research on Hepatitis C has been very successful and has led to multiple research awards, including the 'Equity in Prevention and Treatment Award” from the New York Department of Health Viral Hepatitis Symposium (2018) and the 'Presidential Poster Award” awarded to him by the American College of Gastroenterology (2018). He was also awarded 'Outstanding Clinician in General Medicine” by Venus International Foundation for his extensive research expertise and services, perform over and above the standard expected in the advancement of healthcare, patient safety and quality of care.",institutionString:"Interfaith Medical Center",institution:{name:"Interfaith Medical Center",country:{name:"United States of America"}}},{id:"93517",title:"Dr.",name:"Clement",middleName:"Adebajo",surname:"Meseko",slug:"clement-meseko",fullName:"Clement Meseko",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/93517/images/system/93517.jpg",biography:"Dr. Clement Meseko obtained DVM and PhD degree in Veterinary Medicine and Virology respectively. He has worked for over 20 years in both private and public sectors including the academia, contributing to knowledge and control of infectious disease. Through the application of epidemiological skill, classical and molecular virological skills, he investigates viruses of economic and public health importance for the mitigation of the negative impact on people, animal and the environment in the context of Onehealth. \r\nDr. Meseko’s field experience on animal and zoonotic diseases and pathogen dynamics at the human-animal interface over the years shaped his carrier in research and scientific inquiries. He has been part of the investigation of Highly Pathogenic Avian Influenza incursions in sub Saharan Africa and monitors swine Influenza (Pandemic influenza Virus) agro-ecology and potential for interspecies transmission. He has authored and reviewed a number of journal articles and book chapters.",institutionString:"National Veterinary Research Institute",institution:{name:"National Veterinary Research Institute",country:{name:"Nigeria"}}},{id:"158026",title:"Prof.",name:"Shailendra K.",middleName:null,surname:"Saxena",slug:"shailendra-k.-saxena",fullName:"Shailendra K. Saxena",position:null,profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bRET3QAO/Profile_Picture_2022-05-10T10:10:26.jpeg",biography:"Professor Dr. Shailendra K. Saxena is a vice dean and professor at King George's Medical University, Lucknow, India. His research interests involve understanding the molecular mechanisms of host defense during human viral infections and developing new predictive, preventive, and therapeutic strategies for them using Japanese encephalitis virus (JEV), HIV, and emerging viruses as a model via stem cell and cell culture technologies. His research work has been published in various high-impact factor journals (Science, PNAS, Nature Medicine) with a high number of citations. He has received many awards and honors in India and abroad including various Young Scientist Awards, BBSRC India Partnering Award, and Dr. JC Bose National Award of Department of Biotechnology, Min. of Science and Technology, Govt. of India. Dr. Saxena is a fellow of various international societies/academies including the Royal College of Pathologists, United Kingdom; Royal Society of Medicine, London; Royal Society of Biology, United Kingdom; Royal Society of Chemistry, London; and Academy of Translational Medicine Professionals, Austria. He was named a Global Leader in Science by The Scientist. He is also an international opinion leader/expert in vaccination for Japanese encephalitis by IPIC (UK).",institutionString:"King George's Medical University",institution:{name:"King George's Medical University",country:{name:"India"}}},{id:"94928",title:"Dr.",name:"Takuo",middleName:null,surname:"Mizukami",slug:"takuo-mizukami",fullName:"Takuo Mizukami",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/94928/images/6402_n.jpg",biography:null,institutionString:null,institution:{name:"National Institute of Infectious Diseases",country:{name:"Japan"}}},{id:"233433",title:"Dr.",name:"Yulia",middleName:null,surname:"Desheva",slug:"yulia-desheva",fullName:"Yulia Desheva",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/233433/images/system/233433.png",biography:"Dr. Yulia Desheva is a leading researcher at the Institute of Experimental Medicine, St. Petersburg, Russia. 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In recent years, the application of chemistry to biological molecules has gained significant interest in medicinal and pharmacological studies. This topic will be devoted to understanding the interplay between biomolecules and chemical compounds, their structure and function, and their potential applications in related fields. Being a part of the biochemistry discipline, the ideas and concepts that have emerged from Chemical Biology have affected other related areas. This topic will closely deal with all emerging trends in this discipline.",annualVolume:11411,isOpenForSubmission:!0,coverUrl:"https://cdn.intechopen.com/series_topics/covers/15.jpg",editor:{id:"441442",title:"Dr.",name:"Şükrü",middleName:null,surname:"Beydemir",fullName:"Şükrü Beydemir",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0033Y00003GsUoIQAV/Profile_Picture_1634557147521",institutionString:null,institution:{name:"Anadolu University",institutionURL:null,country:{name:"Turkey"}}},editorTwo:{id:"13652",title:"Prof.",name:"Deniz",middleName:null,surname:"Ekinci",fullName:"Deniz Ekinci",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002aYLT1QAO/Profile_Picture_1634557223079",institutionString:null,institution:{name:"Ondokuz Mayıs University",institutionURL:null,country:{name:"Turkey"}}},editorThree:null,editorialBoard:[{id:"241413",title:"Dr.",name:"Azhar",middleName:null,surname:"Rasul",fullName:"Azhar Rasul",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bRT1oQAG/Profile_Picture_1635251978933",institutionString:null,institution:{name:"Government College University, Faisalabad",institutionURL:null,country:{name:"Pakistan"}}},{id:"178316",title:"Ph.D.",name:"Sergey",middleName:null,surname:"Sedykh",fullName:"Sergey Sedykh",profilePictureURL:"https://mts.intechopen.com/storage/users/178316/images/system/178316.jfif",institutionString:null,institution:{name:"Novosibirsk State University",institutionURL:null,country:{name:"Russia"}}}]},{id:"17",title:"Metabolism",keywords:"Biomolecules Metabolism, Energy Metabolism, Metabolic Pathways, Key Metabolic Enzymes, Metabolic Adaptation",scope:"Metabolism is frequently defined in biochemistry textbooks as the overall process that allows living systems to acquire and use the free energy they need for their vital functions or the chemical processes that occur within a living organism to maintain life. Behind these definitions are hidden all the aspects of normal and pathological functioning of all processes that the topic ‘Metabolism’ will cover within the Biochemistry Series. Thus all studies on metabolism will be considered for publication.",annualVolume:11413,isOpenForSubmission:!0,coverUrl:"https://cdn.intechopen.com/series_topics/covers/17.jpg",editor:{id:"138626",title:"Dr.",name:"Yannis",middleName:null,surname:"Karamanos",fullName:"Yannis Karamanos",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002g6Jv2QAE/Profile_Picture_1629356660984",institutionString:null,institution:{name:"Artois University",institutionURL:null,country:{name:"France"}}},editorTwo:null,editorThree:null,editorialBoard:[{id:"243049",title:"Dr.",name:"Anca",middleName:null,surname:"Pantea Stoian",fullName:"Anca Pantea Stoian",profilePictureURL:"https://mts.intechopen.com/storage/users/243049/images/system/243049.jpg",institutionString:null,institution:{name:"Carol Davila University of Medicine and Pharmacy",institutionURL:null,country:{name:"Romania"}}},{id:"203824",title:"Dr.",name:"Attilio",middleName:null,surname:"Rigotti",fullName:"Attilio Rigotti",profilePictureURL:"//cdnintech.com/web/frontend/www/assets/author.svg",institutionString:null,institution:{name:"Pontifical Catholic University of Chile",institutionURL:null,country:{name:"Chile"}}},{id:"300470",title:"Dr.",name:"Yanfei (Jacob)",middleName:null,surname:"Qi",fullName:"Yanfei (Jacob) Qi",profilePictureURL:"https://mts.intechopen.com/storage/users/300470/images/system/300470.jpg",institutionString:null,institution:{name:"Centenary Institute of Cancer Medicine and Cell Biology",institutionURL:null,country:{name:"Australia"}}}]},{id:"18",title:"Proteomics",keywords:"Mono- and Two-Dimensional Gel Electrophoresis (1-and 2-DE), Liquid Chromatography (LC), Mass Spectrometry/Tandem Mass Spectrometry (MS; MS/MS), Proteins",scope:"With the recognition that the human genome cannot provide answers to the etiology of a disorder, changes in the proteins expressed by a genome became a focus in research. Thus proteomics, an area of research that detects all protein forms expressed in an organism, including splice isoforms and post-translational modifications, is more suitable than genomics for a comprehensive understanding of the biochemical processes that govern life. The most common proteomics applications are currently in the clinical field for the identification, in a variety of biological matrices, of biomarkers for diagnosis and therapeutic intervention of disorders. From the comparison of proteomic profiles of control and disease or different physiological states, which may emerge, changes in protein expression can provide new insights into the roles played by some proteins in human pathologies. Understanding how proteins function and interact with each other is another goal of proteomics that makes this approach even more intriguing. Specialized technology and expertise are required to assess the proteome of any biological sample. Currently, proteomics relies mainly on mass spectrometry (MS) combined with electrophoretic (1 or 2-DE-MS) and/or chromatographic techniques (LC-MS/MS). MS is an excellent tool that has gained popularity in proteomics because of its ability to gather a complex body of information such as cataloging protein expression, identifying protein modification sites, and defining protein interactions. The Proteomics topic aims to attract contributions on all aspects of MS-based proteomics that, by pushing the boundaries of MS capabilities, may address biological problems that have not been resolved yet.",annualVolume:11414,isOpenForSubmission:!0,coverUrl:"https://cdn.intechopen.com/series_topics/covers/18.jpg",editor:{id:"200689",title:"Prof.",name:"Paolo",middleName:null,surname:"Iadarola",fullName:"Paolo Iadarola",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bSCl8QAG/Profile_Picture_1623568118342",institutionString:null,institution:{name:"University of Pavia",institutionURL:null,country:{name:"Italy"}}},editorTwo:{id:"201414",title:"Dr.",name:"Simona",middleName:null,surname:"Viglio",fullName:"Simona Viglio",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bRKDHQA4/Profile_Picture_1630402531487",institutionString:null,institution:{name:"University of Pavia",institutionURL:null,country:{name:"Italy"}}},editorThree:null,editorialBoard:[{id:"72288",title:"Dr.",name:"Arli Aditya",middleName:null,surname:"Parikesit",fullName:"Arli Aditya Parikesit",profilePictureURL:"https://mts.intechopen.com/storage/users/72288/images/system/72288.jpg",institutionString:null,institution:{name:"Indonesia International Institute for Life Sciences",institutionURL:null,country:{name:"Indonesia"}}},{id:"40928",title:"Dr.",name:"Cesar",middleName:null,surname:"Lopez-Camarillo",fullName:"Cesar Lopez-Camarillo",profilePictureURL:"https://mts.intechopen.com/storage/users/40928/images/3884_n.png",institutionString:null,institution:{name:"Universidad Autónoma de la Ciudad de México",institutionURL:null,country:{name:"Mexico"}}},{id:"81926",title:"Dr.",name:"Shymaa",middleName:null,surname:"Enany",fullName:"Shymaa Enany",profilePictureURL:"https://mts.intechopen.com/storage/users/81926/images/system/81926.png",institutionString:"Suez Canal University",institution:{name:"Suez Canal University",institutionURL:null,country:{name:"Egypt"}}}]}]}},libraryRecommendation:{success:null,errors:{},institutions:[]},route:{name:"profile.detail",path:"/profiles/264141",hash:"",query:{},params:{id:"264141"},fullPath:"/profiles/264141",meta:{},from:{name:null,path:"/",hash:"",query:{},params:{},fullPath:"/",meta:{}}}},function(){var e;(e=document.currentScript||document.scripts[document.scripts.length-1]).parentNode.removeChild(e)}()