Spectral parameters for simulations
\\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\\nOur 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\\nAdditionally, each book published by IntechOpen contains original content and research findings.
\\n\\nWe 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"}]',published:!0,mainMedia:{caption:"IntechOpen Maintains",originalUrl:"/media/original/113"}},components:[{type:"htmlEditorComponent",content:'
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\nSimba 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.
\n\nIntechOpen, 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\nSince the first Open Access Book Publishing report published in 2016, IntechOpen has held the top stop each year.
\n\n\n\nMore 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\nOur 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\nAdditionally, each book published by IntechOpen contains original content and research findings.
\n\nWe 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:"7147",leadTitle:null,fullTitle:"Demystifying Polyneuropathy - Recent Advances and New Directions",title:"Demystifying Polyneuropathy",subtitle:"Recent Advances and New Directions",reviewType:"peer-reviewed",abstract:"Knowledge of the structure and function of the complex and interwoven network of nerves is inexhaustible and has not been fully determined. The physiological basis of many neuropathic symptoms continues to pursue experts in this field, and in many of the pathological changes related to neuropathies. In the last few decades, there has been increasing interest in new tools applied to diseases involving nerves of the nervous system, which have changed this state of affairs. Microscopic studies, new quantitative histometric methods, and refined physiologic techniques have already expanded our knowledge of structure and function of nerves and rapidly advancing techniques in the fields of immunology and molecular genetics to clarify entire categories of polyneuropathy. Although polyneuropathy is among the most challenging categories of neurological diseases, effective forms of treatment for polyneuropathy have been introduced during the last few decades. This book intends to provide the reader with a broad overview of polyneuropathy, featuring considerations and diagnostic approaches to patients, specific neuropathic syndromes and new related entities, pathogenic mechanisms, and pathological reactions brought to bear to the therapeutic and new clinical applications. All this is important evidence to support present and future directions in this challenging topic.",isbn:"978-1-83881-192-1",printIsbn:"978-1-83881-191-4",pdfIsbn:"978-1-83881-193-8",doi:"10.5772/intechopen.73946",price:100,priceEur:109,priceUsd:129,slug:"demystifying-polyneuropathy-recent-advances-and-new-directions",numberOfPages:94,isOpenForSubmission:!1,isInWos:null,isInBkci:!1,hash:"884b3c36ad0b0856066a901d2f910ef5",bookSignature:"Patricia Bozzetto Ambrosi",publishedDate:"July 24th 2019",coverURL:"https://cdn.intechopen.com/books/images_new/7147.jpg",numberOfDownloads:5371,numberOfWosCitations:1,numberOfCrossrefCitations:4,numberOfCrossrefCitationsByBook:0,numberOfDimensionsCitations:7,numberOfDimensionsCitationsByBook:0,hasAltmetrics:0,numberOfTotalCitations:12,isAvailableForWebshopOrdering:!0,dateEndFirstStepPublish:"April 10th 2018",dateEndSecondStepPublish:"May 23rd 2018",dateEndThirdStepPublish:"July 22nd 2018",dateEndFourthStepPublish:"October 10th 2018",dateEndFifthStepPublish:"December 9th 2018",currentStepOfPublishingProcess:5,indexedIn:"1,2,3,4,5,6",editedByType:"Edited by",kuFlag:!1,featuredMarkup:null,editors:[{id:"221787",title:"Dr.",name:"Patricia",middleName:null,surname:"Bozzetto Ambrosi",slug:"patricia-bozzetto-ambrosi",fullName:"Patricia Bozzetto Ambrosi",profilePictureURL:"https://mts.intechopen.com/storage/users/221787/images/system/221787.jfif",biography:"Prof. Dr. Patricia Bozzetto Ambrosi graduated with degrees in Medicine from the University of Caxias do Sul, Brazil, and the University of Rome Tor Vergata, Italy. She is a former researcher in morphophysiology at the University of Córdoba/Reina Sofia Hospital, Córdoba, Spain. She graduated in Neurology/Neurosurgery at the Hospital of Restauração, SES, Brazil, and Neuroradiology/Radiodiagnostics at Pierre and Marie Curie University, France. She holds a master’s degree in Medicine from the University of Nova Lisboa, Portugal, and in Behavioral Sciences and Neuropsychiatry from the University of Pernambuco, Brazil. She also has a Ph.D. in Biological Sciences from the University of Pernambuco/Paris Diderot University, France. She is a former fellow in Interventional Neuroradiology in France at the Ophthalmological Foundation Adolphe de Rothschild, Beaujon Hospital, and Hospices Civils de Strasbourg. She was Praticien Associé in Interventional Neuroradiology at Neurologique Hospital Pierre Wertheimer, University of Lyon Claude Bernard, France, and visiting professor of the University of Paris Diderot-Neuri Beaujon. Dr. Ambrosi is an independent consultant/supervisor in neurology, neuroradiology, neuroendovascular, and imaging, and a clinical professor of medicine. She has also been an academic collaborator researcher in the Cardiovascular Department, University of Leicester, England. She has experience in innovative research for the development of new technologies and neurosciences. She is also an academic editor and reviewer of several scientific publications about neurological diseases.",institutionString:"Independent Neuroradiologist and Neurologist Consultant",position:null,outsideEditionCount:0,totalCites:0,totalAuthoredChapters:"1",totalChapterViews:"0",totalEditedBooks:"3",institution:{name:"Paris Diderot University",institutionURL:null,country:{name:"France"}}}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null,coeditorOne:null,coeditorTwo:null,coeditorThree:null,coeditorFour:null,coeditorFive:null,topics:[{id:"1056",title:"Neurology",slug:"neurology"}],chapters:[{id:"64150",title:"The Cutaneous Biopsy for the Diagnosis of Peripheral Neuropathies: Meissner’s Corpuscles and Merkel’s Cells",doi:"10.5772/intechopen.81687",slug:"the-cutaneous-biopsy-for-the-diagnosis-of-peripheral-neuropathies-meissner-s-corpuscles-and-merkel-s",totalDownloads:889,totalCrossrefCites:0,totalDimensionsCites:2,hasAltmetrics:0,abstract:"Cutaneous biopsy is a complementary method, alternative to peripheral nerve biopsy, for the analysis of nerve involvement in peripheral neuropathies, systemic diseases, and several pathologies of the central nervous system. Most of these neuropathological studies were focused on the intraepithelial nerve fibers (thin-myelinated Aδ fibers and unmyelinated C fibers), and few studies investigated the variations in dermal innervation, that is, large myelinated fibers, Merkel’s cell-neurite complexes, and Meissner’s corpuscles. Here, we updated and summarized the current data about the quantitative and qualitative changes that undergo MCs and MkCs in peripheral neuropathies. Moreover, we provide a comprehensive rationale to include MCs in the study of cutaneous biopsies when analyzing the peripheral neuropathies and aim to provide a protocol to study them.",signatures:"Olivia García-Suárez, Yolanda García-Mesa, Jorge García-Piqueras, Giuseppina Salvo, Juan L. Cobo, Elda Alba, Ramón Cobo, Jorge Feito and José A. Vega",downloadPdfUrl:"/chapter/pdf-download/64150",previewPdfUrl:"/chapter/pdf-preview/64150",authors:[{id:"59892",title:"Prof.",name:"José A.",surname:"Vega",slug:"jose-a.-vega",fullName:"José A. Vega"},{id:"270068",title:"Dr.",name:"Yolanda",surname:"Garcia-Mesa",slug:"yolanda-garcia-mesa",fullName:"Yolanda Garcia-Mesa"},{id:"270069",title:"Dr.",name:"Jorge",surname:"Garcia-Piqueras",slug:"jorge-garcia-piqueras",fullName:"Jorge Garcia-Piqueras"},{id:"270070",title:"Dr.",name:"Giussepina",surname:"Salvo",slug:"giussepina-salvo",fullName:"Giussepina Salvo"},{id:"270071",title:"Prof.",name:"Juan L.",surname:"Cobo",slug:"juan-l.-cobo",fullName:"Juan L. Cobo"},{id:"270087",title:"Prof.",name:"Olivia",surname:"García-Suarez",slug:"olivia-garcia-suarez",fullName:"Olivia García-Suarez"},{id:"270088",title:"Dr.",name:"Elda",surname:"Alba",slug:"elda-alba",fullName:"Elda Alba"},{id:"270089",title:"Dr.",name:"Jorge",surname:"Feito",slug:"jorge-feito",fullName:"Jorge Feito"}],corrections:null},{id:"63691",title:"HIV-Associated Sensory Neuropathy",doi:"10.5772/intechopen.81176",slug:"hiv-associated-sensory-neuropathy",totalDownloads:907,totalCrossrefCites:1,totalDimensionsCites:1,hasAltmetrics:0,abstract:"As advances in the treatment of HIV are now allowing patients a longer life span, further comorbidities become apparent. This includes sensory neuropathy (HIV-SN) which can affect a patient’s quality of life. Here, we review factors influencing HIV-SN in patients receiving antiretroviral therapy that promotes this condition and in the modern era when these therapies have been withdrawn. This has halved the incidence of HIV-SN, but the condition remains significant in the lives of many sufferers. Genetic polymorphisms that influence pathogenesis of HIV-SN have indicated likely mechanisms, but studies of skin biopsies and animal models are needed to confirm the roles of the encoded proteins.",signatures:"Fitri Octaviana, Ahmad Yanuar Safri, Darma Imran and Patricia Price",downloadPdfUrl:"/chapter/pdf-download/63691",previewPdfUrl:"/chapter/pdf-preview/63691",authors:[{id:"258946",title:"Dr.",name:"Fitri",surname:"Octaviana",slug:"fitri-octaviana",fullName:"Fitri Octaviana"},{id:"259642",title:"Mr.",name:"Ahmad Yanuar",surname:"Safri",slug:"ahmad-yanuar-safri",fullName:"Ahmad Yanuar Safri"},{id:"259643",title:"Mr.",name:"Darma",surname:"Imran",slug:"darma-imran",fullName:"Darma Imran"},{id:"259644",title:"Prof.",name:"Patricia",surname:"Price",slug:"patricia-price",fullName:"Patricia Price"}],corrections:null},{id:"64691",title:"Peripheral Neuropathy in Connective Tissue Diseases",doi:"10.5772/intechopen.82271",slug:"peripheral-neuropathy-in-connective-tissue-diseases",totalDownloads:1260,totalCrossrefCites:2,totalDimensionsCites:2,hasAltmetrics:0,abstract:"Connective tissue diseases are characterized by different organ disorders due to loss of immune system tolerance to autoantigens. Peripheral neuropathy is one of the features of these diseases with variable frequency; it is more prevalent in Sjögren syndrome. Peripheral neuropathy is often seen in the course of the disease. Nonetheless, it may be also a presenting sign or the unique feature of immune system dysfunction. Neuropathies in connective tissue diseases are related mainly to vasculitic disorder. It requires prompt diagnosis and treatment to improve its outcome. Peripheral neuropathy in connective tissue diseases could be multifocal and asymmetric, or confluent and symmetrical. This chapter reviews the clinical, diagnostic and therapeutic features of neuropathies associated with the common diffuse connective tissue diseases.",signatures:"Mouna Snoussi, Faten Frikha and Zouhir Bahloul",downloadPdfUrl:"/chapter/pdf-download/64691",previewPdfUrl:"/chapter/pdf-preview/64691",authors:[{id:"255819",title:"Dr.",name:"Mouna",surname:"Snoussi",slug:"mouna-snoussi",fullName:"Mouna Snoussi"},{id:"267569",title:"Dr.",name:"Faten",surname:"Frikha",slug:"faten-frikha",fullName:"Faten Frikha"},{id:"267570",title:"Dr.",name:"Zouhir",surname:"Bahloul",slug:"zouhir-bahloul",fullName:"Zouhir Bahloul"}],corrections:null},{id:"68039",title:"Working Hand Syndrome: A New Definition of Nonclassified Polyneuropathy Condition",doi:"10.5772/intechopen.81966",slug:"working-hand-syndrome-a-new-definition-of-nonclassified-polyneuropathy-condition",totalDownloads:718,totalCrossrefCites:0,totalDimensionsCites:0,hasAltmetrics:0,abstract:"The aim of this chapter was to define an unexplained nonclassified polyneuropathy condition as a new neurological disease. This new diagnosis of occupation-related polyneuropathy has been named as “working hand syndrome (WHS).” This study collected and compared clinical and electrophysiological analyses data from healthy controls, WHS patients, carpal tunnel syndrome (CTS) patients, and polyneuropathy patients. The WHS patients presented to the clinic with pain, numbness, tingling, and burning sensations in their hands that increased significantly during rest and nighttime. However, there was no weakness in the muscles, and the deep tendon reflexes were normal in this disease. The patients had all been working in physically demanding jobs requiring the use of their hands/arms for at least 1 year, but no vibrating tools were used by the patients. All of the cases were men. I suppose that overload caused by an action repeated chronically by the hand/arm may impair the sensory nerves in mentioned hand/arm. In patients with these complaints, for a definitive diagnosis, similar diseases must be excluded. Nonetheless, the specific electrophysiological finding that the sural nerves are normal on the lower sides, as well as the occurrence of sensory axonal polyneuropathy in the sensory nerves without a significant effect on velocity and latency in the work-ups of the upper extremity are enough to make a diagnosis.",signatures:"Gökhan Özdemir",downloadPdfUrl:"/chapter/pdf-download/68039",previewPdfUrl:"/chapter/pdf-preview/68039",authors:[{id:"254030",title:"Dr.",name:"Gokhan",surname:"Ozdemir",slug:"gokhan-ozdemir",fullName:"Gokhan Ozdemir"}],corrections:null},{id:"63566",title:"Platelet-Rich Plasma for Injured Peripheral Nerves: Biological Repair Process and Clinical Application Guidelines",doi:"10.5772/intechopen.81104",slug:"platelet-rich-plasma-for-injured-peripheral-nerves-biological-repair-process-and-clinical-applicatio",totalDownloads:1597,totalCrossrefCites:1,totalDimensionsCites:2,hasAltmetrics:0,abstract:"Platelet-rich plasma (PRP) is a biological therapy that uses the patient’s own blood to obtain products with a higher platelet concentration than in blood. It provides a transient fibrin scaffold as a controlled drug delivery system of growth factors suitable for regenerative medicine. PRP has been used as medical strategy to treat diverse types of injuries in the field of orthopedics, including peripheral nerve lesions. In vitro and in vivo studies showed the neuroprotective, neurogenic and neuroinflammatory modulator effect of PRP. In addition, it has been demonstrated clinically that PRP infiltrations improve clinical symptoms and enhance the sensory and motor functional nerve muscle unit recovery. Potential effects of PRP could be applied in treatments for neuropathies, as conservative treatment by means of nerve ultrasound-guided infiltrations or as biological adjuvant during surgery.",signatures:"Mikel Sánchez, Ane Garate, Ane Miren Bilbao, Jaime Oraa, Fernando Yangüela, Pello Sánchez, Jorge Guadilla, Beatriz Aizpurua, Juan Azofra, Nicolás Fiz and Diego Delgado",downloadPdfUrl:"/chapter/pdf-download/63566",previewPdfUrl:"/chapter/pdf-preview/63566",authors:[{id:"208758",title:"M.D.",name:"Mikel",surname:"Sánchez",slug:"mikel-sanchez",fullName:"Mikel Sánchez"},{id:"208807",title:"Dr.",name:"Nicolás",surname:"Fiz",slug:"nicolas-fiz",fullName:"Nicolás Fiz"},{id:"208808",title:"Dr.",name:"Juan",surname:"Azofra",slug:"juan-azofra",fullName:"Juan Azofra"},{id:"208809",title:"Dr.",name:"Jaime",surname:"Oraa",slug:"jaime-oraa",fullName:"Jaime Oraa"},{id:"208810",title:"Dr.",name:"Ane",surname:"Garate",slug:"ane-garate",fullName:"Ane Garate"},{id:"208812",title:"MSc.",name:"Pello",surname:"Sánchez",slug:"pello-sanchez",fullName:"Pello Sánchez"},{id:"208813",title:"Dr.",name:"Diego",surname:"Delgado",slug:"diego-delgado",fullName:"Diego Delgado"},{id:"228711",title:"Dr.",name:"Ane Miren",surname:"Bilbao",slug:"ane-miren-bilbao",fullName:"Ane Miren Bilbao"},{id:"228712",title:"Dr.",name:"Jorge",surname:"Guadilla",slug:"jorge-guadilla",fullName:"Jorge Guadilla"},{id:"228713",title:"Dr.",name:"Beatriz",surname:"Aizpurua",slug:"beatriz-aizpurua",fullName:"Beatriz Aizpurua"},{id:"254161",title:"Dr.",name:"Fernando",surname:"Yangüela",slug:"fernando-yanguela",fullName:"Fernando Yangüela"}],corrections:null}],productType:{id:"1",title:"Edited Volume",chapterContentType:"chapter",authoredCaption:"Edited by"},subseries:null,tags:null},relatedBooks:[{type:"book",id:"9364",title:"New Insight into Cerebrovascular Diseases",subtitle:"An Updated Comprehensive 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\r\n\t“Citizen Science - Methods, Approaches and New Perspectives” intends to give a comprehensive account of theoretical and practical aspects of Public Participation in Scientific Research. In recent years, citizen science has been rapidly expanding worldwide. This book will cover several important topics in Citizen science. Topics discussed include, but are not limited to: public understanding of science, government policies, crowdsourcing, open Science, science-society relationship, citizen science monitoring programmes, and case studies in public engagement in scientific research. It will interest a wide range of readers, including policymakers, volunteers, scientists, specialists, and students involved in citizen science projects research or who would like to design and lead their own projects. The relationship between science and the public is central to the constitution of contemporary societies. In an era when pressing environmental issues, cooperation across science and society is crucial, and this book will present a collaborative analysis by experts from different academic fields.
",isbn:"978-1-83768-317-8",printIsbn:"978-1-83768-316-1",pdfIsbn:"978-1-83768-318-5",doi:null,price:0,priceEur:0,priceUsd:0,slug:null,numberOfPages:0,isOpenForSubmission:!0,isSalesforceBook:!1,isNomenclature:!1,hash:"655a28c11339d0891d964ca336d4e076",bookSignature:"Dr. Alessio Vovlas",publishedDate:null,coverURL:"https://cdn.intechopen.com/books/images_new/12250.jpg",keywords:"Crowdsourcing, Citizen Collected Data, Open Science, Public Understanding of Science, Government Policies, Biodiversity, Astronomy, Seismology, Health and Welfare, Pollution, Environmental Monitoring, Taxonomy",numberOfDownloads:null,numberOfWosCitations:0,numberOfCrossrefCitations:null,numberOfDimensionsCitations:null,numberOfTotalCitations:null,isAvailableForWebshopOrdering:!0,dateEndFirstStepPublish:"June 3rd 2022",dateEndSecondStepPublish:"July 1st 2022",dateEndThirdStepPublish:"August 30th 2022",dateEndFourthStepPublish:"November 18th 2022",dateEndFifthStepPublish:"January 17th 2023",dateConfirmationOfParticipation:null,remainingDaysToSecondStep:"13 hours",secondStepPassed:!0,areRegistrationsClosed:!1,currentStepOfPublishingProcess:3,editedByType:null,kuFlag:!1,biosketch:"Alessio Vovlas has worked in the past on the ecology and biodiversity of butterflies and now is currently a Research Assistant at Italian National Research Council in Bari (Italy) in Nematology, and is a member of the International Union for Conservation of Nature (IUCN) and the Society for Conservation Biology.",coeditorOneBiosketch:null,coeditorTwoBiosketch:null,coeditorThreeBiosketch:null,coeditorFourBiosketch:null,coeditorFiveBiosketch:null,editors:[{id:"313084",title:"Dr.",name:"Alessio",middleName:null,surname:"Vovlas",slug:"alessio-vovlas",fullName:"Alessio Vovlas",profilePictureURL:"https://mts.intechopen.com/storage/users/313084/images/system/313084.png",biography:"Alessio Vovlas received a Ph.D. in Science and Technology from Turin University, Italy, in 2014 with a thesis on 'Evolutionary Biology and Biodiversity Conservation,” and an MS in Natural Science from Bari University, Italy, He is an effective member of A.P.S. Polyxena, an NGO that is part of the Butterfly Conservation Europe, European Citizen Science Association (ECSA), and Societas Europaea Lepidopterologica (SEL). He is also a member of the Society for Conservation Biology and part of the membership committee of the International Union for Conservation of Nature (IUCN) Commission on Education and Communication (CEC). Dr. Vovlas’ main research interests are molecular biology, ecology, zoology, science communication, and education. He has published several scientific, national, and international publications and was a coordinator of some nature conservation and citizen science projects in natural park areas.",institutionString:"National Research Council",position:null,outsideEditionCount:0,totalCites:0,totalAuthoredChapters:"2",totalChapterViews:"0",totalEditedBooks:"1",institution:{name:"National Research Council",institutionURL:null,country:{name:"Italy"}}}],coeditorOne:null,coeditorTwo:null,coeditorThree:null,coeditorFour:null,coeditorFive:null,topics:[{id:"23",title:"Social Sciences",slug:"social-sciences"}],chapters:null,productType:{id:"1",title:"Edited Volume",chapterContentType:"chapter",authoredCaption:"Edited by"},personalPublishingAssistant:{id:"453623",firstName:"Silvia",lastName:"Sabo",middleName:null,title:"Mrs.",imageUrl:"https://mts.intechopen.com/storage/users/453623/images/20396_n.jpg",email:"silvia@intechopen.com",biography:null}},relatedBooks:[{type:"book",id:"6942",title:"Global Social Work",subtitle:"Cutting Edge Issues and Critical Reflections",isOpenForSubmission:!1,hash:"222c8a66edfc7a4a6537af7565bcb3de",slug:"global-social-work-cutting-edge-issues-and-critical-reflections",bookSignature:"Bala Raju Nikku",coverURL:"https://cdn.intechopen.com/books/images_new/6942.jpg",editedByType:"Edited by",editors:[{id:"263576",title:"Dr.",name:"Bala",surname:"Nikku",slug:"bala-nikku",fullName:"Bala Nikku"}],productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"6926",title:"Biological Anthropology",subtitle:"Applications and Case Studies",isOpenForSubmission:!1,hash:"5bbb192dffd37a257febf4acfde73bb8",slug:"biological-anthropology-applications-and-case-studies",bookSignature:"Alessio Vovlas",coverURL:"https://cdn.intechopen.com/books/images_new/6926.jpg",editedByType:"Edited by",editors:[{id:"313084",title:"Dr.",name:"Alessio",surname:"Vovlas",slug:"alessio-vovlas",fullName:"Alessio Vovlas"}],productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"1591",title:"Infrared Spectroscopy",subtitle:"Materials Science, Engineering and Technology",isOpenForSubmission:!1,hash:"99b4b7b71a8caeb693ed762b40b017f4",slug:"infrared-spectroscopy-materials-science-engineering-and-technology",bookSignature:"Theophile Theophanides",coverURL:"https://cdn.intechopen.com/books/images_new/1591.jpg",editedByType:"Edited by",editors:[{id:"37194",title:"Dr.",name:"Theophile",surname:"Theophanides",slug:"theophile-theophanides",fullName:"Theophile Theophanides"}],productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"3161",title:"Frontiers in Guided Wave Optics and Optoelectronics",subtitle:null,isOpenForSubmission:!1,hash:"deb44e9c99f82bbce1083abea743146c",slug:"frontiers-in-guided-wave-optics-and-optoelectronics",bookSignature:"Bishnu Pal",coverURL:"https://cdn.intechopen.com/books/images_new/3161.jpg",editedByType:"Edited by",editors:[{id:"4782",title:"Prof.",name:"Bishnu",surname:"Pal",slug:"bishnu-pal",fullName:"Bishnu Pal"}],productType:{id:"1",chapterContentType:"chapter",authoredCaption:"Edited by"}},{type:"book",id:"371",title:"Abiotic Stress in Plants",subtitle:"Mechanisms and Adaptations",isOpenForSubmission:!1,hash:"588466f487e307619849d72389178a74",slug:"abiotic-stress-in-plants-mechanisms-and-adaptations",bookSignature:"Arun Shanker and B. 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Irradiation at lower dose levels also extends shelf-life and can be used to control insects. Irradiation extends the shelf-life of food by retarding maturation in vegetables and reducing spoilage organisms that can grow even under refrigeration. Irradiation can also be used in place of fumigants and other quarantine procedures to import or export fruits and vegetables without the risk of transporting harmful insects.
Electron spin resonance (ESR) studies have reported on induced radicals in irradiated plant foods (Ukai et al., 2006; Ukai & Shimoyama, 2003a, 2003b, 2005; Nakamura et al., 2006; Shimoyama et al., 2006). There are two types of ESR signals from irradiated plant food: one is a singlet with a g-value of nearly 2.0, and the other appears symmetrically as two side signals on both sides of the singlet. The singlet signal has been identified as an organic free radical (Ukai & Shimoyama, 2005).
Clear side signals have been reported in pepper following gamma-ray irradiation (Ukai & Shimoyama, 2003a, 2003b). Similar side signals in wheat flour that contains cellulose and starch are more complicated (Shimoyama et al., 2006; Ukai & Shimoyama, 2005). Side signals have been observed in ginseng that contains a significant amount of fiber (Nakamura et al., 2006) and in irradiated strawberry seeds whose main component is cellulose (Raffi & Stocker, 1996; Raffi & Agnel, 1989). However, only one side signal at the lower magnetic fields has been detected (Raffi & Agnel, 1989). The side signal in the higher magnetic field was considered covered by other stronger ESR signals. These side signals have been named after the “cellulotic radical,” because they are observable in ESR spectra of samples containing a significant amount of cellulose (Raffi et al., 2000). Ehrenberg et al. have reported that the side signals appearing from irradiation were derived from peroxide radicals (Loftroth et al., 1964; A. Ehrenberg et al., 1962). There have been many recent reports on the side signals (Lee et al., 2009; Lee et al., 2008; Yordanov et al., 2009; Raffi et al., 2009; Yamaoki et al., 2009; Sanyal et al., 2008; Cutrubinis et al., 2007; Polovka et al., 2007; Jo & Kwon, 2006; Butz & Hildebrand, 2006).
Lee et al. have reported on irradiated sesame seeds using ESR (Lee et al., 2009; Lee et al., 2008). The report concluded that a pair of ESR lines appears on both sides of the central signal in ESR spectra due to the cellulose radicals formed by ionizing radiation. Yordanov et al. have reported a pair of signals in the irradiated dry medical herbs (Yordanov et al., 2009). A central line and two weak satellite lines were detected. The authors named these after the “cellulose-like” and “carbohydrate-like” triplets (Yordanov et al., 2009). However, their spectra were undefined. Raffi and Yordanov have reported on aromatic herbs, spices, and fruits after irradiation (Raffi et al., 2009). They have also reported a relatively weak triplet.
Polovka et al. have reported on irradiated spices (Polovka et al., 2007). Simulation of ESR spectra for the black pepper samples revealed the formation of three paramagnetic species, i.e., the triplet, doublet assigned to “carbohydrate” radical structures, and the typical three-line “cellulotic” signal. The paramagnetic signals identified in individual irradiated spice samples, along with the spin Hamiltonian parameters, have been employed in quasi-empirical simulations.
A triplet line has been reported from the irradiated flesh of kiwifruits, with the extra signals resulting from cellulose radicals on both sides of the endogenous signal (Jo & Kwon, 2006). Studies on the irradiated shells of walnuts and pistachios have shown that a sample can be unambiguously identified, if beside the central signal satellite peaks, a separation of 6.0 ± 0.05 mT is detected (Butz & Hildebrand, 2006). However, there is little explanation on the origin of the side signals.
With the CW-ESR method, irradiation can be performed using a weak (continuous) microwave field without disturbing the steady state spin system. The pulsed-ESR method employs instantaneous microwave radiation and reorients the spin systems. This can be observed in the absence of a microwave field. Pulsed ESR determines the relaxation behavior of radicals. The relaxation times, T1 and T2, were evaluated using the decay of echo signals as a function of time intervals between microwave pulses. However, strict measurement conditions must be met for an accurate analysis of pulsed ESR.
In this study, gamma ray radiation was applied on filter paper that was made of pure cellulose and on an oblate of pure starch which has structure similar to cellulose. We analyzed the ESR side signals originating from these polymers after irradiation. Using theoretical calculations, we simulated the side signals by assuming a triplet signal from the radical at the C(5) position of the glucose unit (Fig. 1 A). This revealed the molecular mechanism of the radical formation. Furthermore, we examined irradiated black pepper using pulsed ESR. Black pepper contains many cellulose and many researchers reported the radicals in irradiated black pepper using ESR. But there is no report of the measurement of irradiated black pepper containing much cellulose using pulsed ESR. We employed an electron spin echo (ESE) using the pulsed ESR method, i.e., the π/2- and π-pulse sequence. We measured the relaxation of the spin system and various magnetic parameters such as the g-value and hyperfine couplings.
The chemical structure of the cellulose radical. A) before irradiation and B) after irradiation. The triplet ESR spectrum of cellulose is due to the interactions between the two hydrogen atoms at the C6 position of the glucose unit with the unpaired electron formed by the removal of the hydrogen atom at the C5 position of the glucose unit by irradiation
Filter paper (ADVANTEC MFS., INC) and oblate (Kokko-Oblate Co., Ltd.) were used as samples. The quality of filter paper and oblate used was more than 90% (Japanese Industrial Standards Committee, 1995) cellulose and 99.2% (Kokko-Oblate Co. Ltd.) starch. Black pepper powder which is one of the foods containing much cellulose, commercially available in Japan, was used in the present study. It was bottled in glass and stored at +4.0 °C. After the samples were obtained, they were carefully sealed in a quartz sample tube (99.9% purity; Eiko, Tokyo, Japan). We prepared sample tubes in an argon (Ar) atmosphere and sealed the tubes to remove any oxygen effects (Nakamura et al., 2006). First, the ESR sample tube was degassed for 5 min, and Ar gas was substituted. Then, Ar gas was purged into the ESR sample five times for 2 min each time. The inside pressure of the ESR tube filled with Ar gas was ca. 1 mmHg.
Irradiation was carried out at the Japan Atomic Energy Research Institute (Takasaki Research Institute) at room temperature (ca. 300 K). We used the gamma-ray originated from 60Co as the irradiation source. The dose rate was 2 kGy/h, and the dose level was controlled by the irradiation time. The irradiation dose levels used were 1, 10, 25, 50, and 100 kGy.
CW-ESR measurements were performed with JES-FA100 (JEOL) at 25 °C using the microwave X-band frequency (9.45 GHz). The field modulation frequency was 100 kHz. For the determination of g-values (Swartz et al., 1972), an Mn marker (JEOL) was employed for the correct microwave frequency. In all ESR measurements pertaining to the present study, the magnetic field was swept in the range of 250.0 ± 250.0 mT with a field modulation of 1.0 mT, time constant of 0.03 s, and sweep time of 4 min. When focusing on the single peak at g = 2.00, the magnetic field was swept over the range of 336.5 ± 7.5 mT, with a time constant of 0.03 s and sweep time of 4 min. The side peaks were detected using smaller noise conditions, comprising a field modulation of 1.0 mT. ESR signal parameters were analyzed using the WIN-RAD (Radical Research) software program.
All pulse-ESR measurements (ESP-380E, Bruker Biospin, Yokohama, Japan) were performed at 25 ◦C. To detect the pulsed electron spin-echo signals, we used a π/2–π pulse sequence. We used 16 ns for the π/2 pulse and 24 ns for the π pulse. The pulse interval was 200 ns; recycle delay, 1 ms; and microwave frequency, 9.480 GHz. The electron spin-echo envelope modulation (ESEEM) was measured at the center of the magnetic field (341.5 mT) of the main peak. Theoretically, when the π/2 pulse is assigned as 16 ns, the corresponding π pulse is 32 ns. We used a shorter pulse, 24 ns, to compensate for the effect of the pin diode on pulse quality. To obtain the echo-detected ESR spectra, the intensity of the electron spin echo was measured as a function of the magnetic field.
The hyperfine data for two Hα in H2Cα-Cβ fragments were obtained from ENDOR data of irradiated malonic acid (Sagstuen et al., 2000). In the first step, we transformed the tensors into the XYZ axes (Z⊥XY-plane) in terms of the two tensor elements AXX and AYY. These were obtained by standard procedures, assuming an angle (30° slightly idealized).
AXX = A1cos2300 + A2sin2300 = -17.95 G
AYY = A1sin2300 + A2cos2300 = -29.05 G
In the second step, rapid rotation about either X or Y was taken into account.
X: The two H˂-tensors both became axially symmetric about X, with A‖ = -17.95 G. One had Trace (A) = A‖ + 2A⊥ = (trace invariant under similarity transformation) = A1 + A2 + A3 = -69.8 G. Therefore, A⊥ = -25.9 G.
Y: The two H˂-tensors became axially symmetric about Y, with A‖ = -29.05 G. By the similar calculation, A⊥ = -20.4 G.
Powder spectra for the two models were simulated by an updated version of the KVAPOL program (Thuomas & Lund, 1976).
To determine T1 and T2, we used Lund’s program (Lund, 2009). For a Gaussian envelope of Lorentzian spin packets, previous treatments have shown the EPR line shape can be expressed as
which is a convolution of a Gaussian line of width t/a and a Lorentzian line of width t, resulting in a Voigt line profile. Here, β is the transition probability of the line g(r) centered at B0. The variables r and r´ are defined by the corresponding magnetic fields B and B´ as
The parameters a and t2 affecting the shape of the saturation curve are given by
ΔBL and ΔBG are the full widths at half maximum value (FWHM) of the unsaturated Lorentzian and Gaussian line shapes, respectively, and can be expressed in terms of the peak-to-peak widths λL and λG of the corresponding 1st derivatives as
The saturation factor s contains the gyromagnetic ratio γ, amplitude of the (left-handed) rotating microwave magnetic field component in the cavity, B1, and spin-lattice and spin-spin relaxation times T1 and T2, respectively. Note that the amplitude B1 is one-half of the amplitude of the linearly polarized field B1 in the resonance resonator, as employed experimentally.
The amplitude B1 of the rotating microwave magnetic field component at the sample position of a microwave resonator is related to the input microwave power by an expression of the type
where the constant K depends on the type of resonator and its quality factor QL (loaded Q) with the sample in place. It may often be difficult to estimate its value precisely.
Substituting the experimentally measured microwave power P and introducing the spin-relaxation-dependent parameter
the absorption line shape of equation (1) can be recast to
where the Voigt profile u is the real part of the complex error function w
The procedure to evaluate the line shape function g(r) (equation (7)) numerically, by expanding the function u(ar,at) as the real part of the complex error function, was outlined previously, and was also used in the present work. The code for the Gautschi algorithm, to calculate a Voigt profile as the real part of the complex error function, is a FORTRAN translation of the original ALGOL procedure. To measure the saturation behavior of a single, inhomogenously broadened line, the transition probability β is set to 1 as in a simple two-level system.
Experimentally, the first derivatives of the absorption spectra are recorded, and therefore, the function g(r) has to be differentiated with respect to the variable r (or magnetic field). This was more conveniently done numerically in this work.
The spin-spin relaxation time T2 is given by definition as
We used two π/2–τ–π pulse sequences at 16 ns and 24 ns for taking echo measurements. The pulse interval was 200 ns, and the recycle delay was 1.0 ms. For each relaxation measurement, we employed a specific pulse sequence. To determine T2, we used a two-pulse sequence:
π/2 pulse–τ–π pulse–τ–(echo)
To determine T1, we used a three-pulse sequence (i.e., the inversion recovery method);
π pulse–τ−π/2 pulse–τ–π pulse–τ–(echo)
We used the same parameter sets as for the spin echo measurements, and fixed τ at 200 ns, to obtain relaxation measurements.
The g-value was determined independently using the position of the magnetic field and the microwave frequency. For accuracy, the values of the magnetic field and frequency were considered out to the fourth and fifth decimal places, respectively.
Figure 2 shows ESR spectra (0 to 500mT) of the filter paper and oblate before and after gamma-ray irradiation. No ESR signals were detected from the two types of samples before irradiation. This suggests the high purity of those samples without an irradiation history.
ESR spectra of filter paper and oblate before and after gamma-irradiation. A: irradiated filter paper, B: filter paper, C: irradiated oblate, and D: oblate.
A strong and sharp singlet signal (P1) was observed near g = 2.0 from the irradiated samples. The g-values of the P1 signal were identified as g = 2.0065 for the filter paper and g = 2.0069 for the oblate. We have already reported on the ESR singlet signal at g = 2.0 using irradiated ginseng (Nakamura et al., 2006) and black pepper (Ukai & Shimoyama, 2003a, 2003b). These irradiated samples showed two kinds of radicals by ESR analysis: Fe3+ at g = 4.0 and Mn2+ hyperfine splitting (Swartz et al., 1971). However, irradiated filter paper and irradiated oblate showed neither the Fe3+ signal nor Mn2+ hyperfine splitting. The signal intensity of P1 measured from the irradiated filter paper was stronger than that from the irradiated oblate.
Figure 3 shows ESR spectra of the filter paper and oblate followed by irradiation at a magnetic field strength of 329 to 344 mT. In the case of the filter paper, S1 and S2 signals were observed at both sides of the P1 signal. The side signals (S1 and S2) were detected at symmetrical positions around the P1 signal. The g-value of the side signals was found to be 2.0241 for S1 and 1.9799 for S2. However, corresponding side signals were not observed in the oblate case.
ESR spectra of filter paper and oblate after irradiation. A: irradiated filter paper and C: irradiated oblate.
Experimental evidence (Figs. 2, 3) shows that side signals only appear in cellulose molecules after irradiation. The two side signals occur simultaneously in the ESR spectrum of cellulose. We observed the side signals disappear simultaneously when increasing temperature (Ukai & Shimoyama, 2003b).
Furthermore, according to a monograph on the ESR studies of irradiated polymers (Rånby, 1977), the majority of references have concluded that, among other candidate radicals, a radical at the C(5) position of the glucose unit is the most plausible one in irradiated cellulose. In general, hydrogen abstraction occurs at various chemical bonds by the gamma-irradiation. All the proton sites undergo various chemical reactions simultaneously. However the radical produced at the C(5) position of the glucose unit was comparably stable, so its ESR signal was observable. The stability of the radical was enhanced by the nearby oxygen and alkyl group at the C(6) position of the glucose unit. The ESR signal of the radical at the C(5) position of the glucose unit yields a triplet line shape due to hyperfine interactions between the unpaired electron of a carbon atom and two protons.
Two side signals (S1 and S2) were detected in irradiated filter paper (containing cellulose), but not in oblate (containing starch). Therefore, we considered that the side signals were from the cellulose and not from starch. We observed side signals induced by irradiation in botanical foods (Ukai & Shimoyama, 2003a, 2003b, 2005; Shimoyama et al., 2006) and crude drugs (Nakamura et al., 2006) containing cellulose.
Filter paper and oblate consist of cellulose and starch, respectively, and both of them are polysaccharides, represented by the chemical formula (C6H10O5)n. Cellulose is a glucose polymer, a β-glucose molecule polymerized by a glycoside bond. Conversely, starch is a polymer produced by polymerizing α-glucose molecules. These structures are different from each other. Cellulose has a sheet-like structure, whereas starch has a helical structure because of the difference in 1, 4 bonds. Thus starch molecules do not form regular sheets and H-bonding is very different. Even though cellulose and starch have similar chemical formulas, their radical formation process may differ due to their structures (Rånby, 1977). It has been reported that the triplet ESR spectrum of cellulose (pure cotton) is due to the equal interaction of the two hydrogen atoms at the C6 position with the unpaired electron formed by the removal of the hydrogen atom at the C5 position of the glucose unit (Rånby, 1977; Arthur, 1971; Arthur & Hinojosa, 1971; Arthur et al., 1966; Baugh et al., 1967) (see Fig. 1 B). The bond breakage at the C5 position may occur only in cellulose. Thus, induction of the side signals should be caused by the strong bonding by β-1, 4 bonds in cellulose.
Upon irradiation, the C5 bond was broken and a radical formed in the cellulose ring (Rånby, 1977). The equivalent two protons located near the unpaired electron at the C5 position of the glucose unit. Thereby, hyperfine interactions occur between the electron spin and the two protons, and the triplet ESR line resulted. The side signals are a part of the triplet. Some interaction between the two protons and the unpaired electron sites at the C2, C3, and C4 positions of the glucose unit are possible, and can be predicted in the cellulose structure (Rånby, 1977; Arthur et al., 1966; Baugh et al., 1967). One needs to consider the physical three-dimensional structure and energy levels of cellulose bond sites. The irradiated starch samples showed a doublet ESR signal (Rånby, 1977; Adamic, 1968). The unpaired electron in the C5 position of the glucose unit produces the doublet-line spectrum by the hyperfine interaction with H5 (Rånby, 1977; Adamic, 1968).
We revealed the origin of the ESR side signals detected from irradiated filter paper containing pure cellulose. Using theoretical calculations, we further revealed the molecular mechanism of the radical formation of irradiated glucose polymers. The side signals are found to be a precise indicator for irradiation effects in cellulose. They originated from neither the peroxide radical of glucose polymers nor the so-called “cellulotic” radicals. By a simulation method, we proved that the side signals originate from a triplet consisting of a hyperfine interaction with two protons, although the main peak is invisible by an overlapping organic free radical at g = 2.0. Note that we reconfirmed that the simulated spin concentration coincides with the experimental ESR value of 1.7 × 1015 spins/g.
Figure 4 shows experimental ESR as well as the simulated ESR spectra of the radical at the C(5) position of the glucose unit. We simulated the ESR spectra under three different conditions of the radical molecule based upon its molecular structure at the C(5) position of the glucose unit. The first is a spectrum at the rigid limit. In the second case, both Cα-Cβ and Cβ-H bonds undergo rapid rotations. For the simulation, we employed a set of magnetic parameters such as hfc and g-value tensors as shown Table 1. We used g = 2.0065 and A = 3.0 mT for the radical at the C(5) position of the glucose unit. Because the experimental ESR spectrum indicated a signal with modified hyperfine values, rather than a powder pattern at the rigid limit, we postulated that the radical undergoes rotational motions. In fact, we found through a simulation that the Cα-Cβ and Cβ-H bonds do undergo simultaneous rotations.
Rigid limit | C-C rotation | C-C rotation and C-H rotation | |
Hyperfine splitting (mT) | Ax = 3.46 | A┴ = 2.00 | A┴ = 2.00 |
Ay = 1.24 | A┴ = 2.00 | A┴ = 2.00 | |
Az = 2.28 | A║ = 2.99 | A║ = 2.99 | |
Line shape ratio (L:G) | 0:100 | 0:100 | 0:100 |
Spectral parameters for simulations
The simulated ESR spectra originated from the radical at the C(5) position of glucose unit under three different conditions of the radical molecule. Experimental ESR spectra of filter paper and oblate after irradiation. A: simulated spectra of rigid limit, B: simulated spectra of C-C rotation, and C: simulated spectra of C-C rotation and C-H rotation.
Figure 5 shows a field-swept echo spectrum (shown from 330.0 to 350.0 mT) of the radicals from gamma-ray-irradiated black pepper. We found three peaks: a main peak and two side peaks. An integrator was not used in the present pulse ESR experiment; therefore, the line width of the main peak detected by pulse-ESR was broader than that of the main peak detected by CW-ESR. The signal intensity of the main peak, at g = 2.005, increased with the radiation dosage. Two side peaks were observed when the irradiation doses were higher than 25 kGy. Black pepper contained much cellulose. So, these peaks are due to irradiated cellulose.
Field-swept (330.0 to 350.0 mT) echo spectrum of gamma-ray-irradiated black pepper at 100 kGy analyzed by pulsed EPR with a microwave frequency of 9.480 GHz. Black pepper powder commercially available in Japan was used. The initial tau value of time between pulses was 200 ns.
The CW-ESR spectra showed 6.0 mT of hyperfine separation between the two side peaks. The field-swept echo yielded a splitting of ca. 6 mT, as shown in Fig. 5. We concluded that both the ESR and the field-swept echo showed the same radical species. We have already reported the corresponding ESR peaks with other specimens using the CW-ESR measurements (Ukai et al., 2006; Ukai & Shimoyama, 2003a, 2003b, 2005; Nakamura et al., 2006; Shimoyama et al., 2006). We observed the same information in the spectra of both pulse- and CW-ESR.
Figure 6 shows a decay signal from the electron spin echo of the gamma-ray-irradiated black pepper sample at the magnetic field position of the main peak (341.5 mT). This echo decay shows ESEEM during the initial time range. ESEEM is also caused by the weak hyperfine interaction between the radiation-induced radicals and remote matrix protons. The two-pulse ESEEM spectra in the present study showed a decay of the observed main peak. The main peak is attributed to oxidized hydroquinone generating paramagnetic semiquinone that exists as an anion or neutral radical. The central peak of the cellulose radical exists in the same position (Kameya et al., 2011).
The peaks in the Fourier-transformed ESEEM spectrum shown in Fig. 6 appeared at 14 MHz and 28 MHz. These peaks are considered to originate from the matrix protons (Astashkin et al., 2000; Gramza et al., 1997). The protons are situated around the radical without being chemically connected. Because this pulse ESR system can detect the interaction between radicals located within a distance of 5 Å, the matrix protons should be situated within 5 Å.
Two-pulse ESEEM time domain spectrum of gamma-ray-irradiated black pepper at 100 kGy with a microwave frequency of 9.480 GHz. Black pepper powder commercially available in Japan was used. The initial tau value of time between pulses was 200 ns.
We measured the relaxation times (T1 and T2) of the radical at 341.5 mT in the black pepper using the pulsed echo sequence. Table 2 summarizes the relaxation times (T1 and T2) of the irradiation-induced radicals in irradiated black pepper. T1 was calculated using exp(-t/T) as the reverse of the spectrum that corresponds to 1-exp (-t/T). T1 of the radical produced by 1 kGy of irradiation was 29.7 µs, and T1 of the radical produced by 100 kGy was 36.0 µs. Relaxation time T2 was calculated using exp (-t/T), and found to be 276 ns for 1 kGy of irradiation, and 437 ns for 100 kGy of gamma-ray-irradiation. Both the T1 and T2 values were enhanced by higher irradiation dosage levels., The relaxation time of the electron spin lattice T1 depends on several parameters, and this relaxation can occur in various ways, e.g., spin diffusion. We expected the relaxation times to decrease because the dipole interaction (the distance between the radicals) weakened with increasing concentration of irradiation-induced radicals. However, the value of T1 increased slightly, possibly because of an energy flow through the chemical bonds resulting from radical formation through irradiation. Relaxation time T2 reflected the interaction among spins. We expected T2 to decrease with increasing concentration of radicals, i.e., interaction between the radicals by gamma-ray irradiation. However, the values of T2 were found to increase with the irradiation dose levels. We believe that this interaction between radicals decreased with conformational changes occurring because of bond breakage, caused in turn by the gamma-ray irradiation.
Pulse-ESR value | CW-ESR value | |||
Irradiateddose(kGy) | T1(×10⌠s) | T2(×102 ns) | T1(⌠s) | T2(×102 ns) |
0 | 3.0 | 2.8 | 3.2 | 1.4 |
1 | 3.0 | 2.9 | 3.3 | 1.5 |
10 | 3.0 | 3.5 | 3.3 | 1.5 |
25 | 3.2 | 3.5 | 3.4 | 1.5 |
50 | 3.3 | 4.2 | 3.4 | 1.6 |
Relaxation times (T1 and T2) of the radiation induced radicals in irradiated black pepper
In this research, we observed relaxation behaviors of the main singlet peak at 341.5 mT. However, from the theoretical analysis of side peaks, we found that the main singlet peak overlaps with the center peak of the triplet (Kameya et al., 2011). These observations suggest that the carbon-centered radical is responsible for the overlapping of peaks and affects the relaxation times, T1 and T2. The relaxation times were also calculated theoretically using the CW-ESR parameter (Lund, 2009). We revealed that T1 and T2 from pulsed-ESR and CW-ESR were changed similarly before and after irradiation.
Relaxation times (T1, T2) of radicals in black pepper were also measured using pulsed-ESR. T1 and T2 were theoretically calculated using the CW-ESR parameter. We used pulsed-ESR and CW-ESR to calculate T1 and T2. T1 and T2 values increased according to irradiation. We revealed that T1 and T2 from pulsed-ESR and CW-ESR were changed similarly before and after irradiation. Before gamma-ray irradiation, no signals were observed in the cellulose. However, after gamma-ray irradiation, a singlet at g = 2.0 was observed, and a pair of side signals appeared simultaneously. Analysis of our theoretical spectra simulation revealed that the hyperfine interactions between the electron spin and the two protons resulted in a triplet ESR line. We compared the experimental spectra with the simulation spectra, and the results corresponded quite closely. We concluded that the twin peaks from the ESR spectra of irradiated cellulose were due to radicals produced at the C(5) site of molecular cellulose.
We detected ESR side signals from irradiated filter paper containing pure cellulose, and revealed the molecular mechanism of the radical formation of irradiated glucose polymers using theoretical calculations. The side signals are a precise indicator for irradiation effects in cellulose.
We postulated that the radical undergoes rotational motions. In simulation, the Cα-Cβ and Cβ-H bonds undergo simultaneous rotations.
We detected the same information in the spectra of both pulse- and CW-ESR. We observed a decay signal from the electron spin echo of the gamma-ray-irradiated black pepper sample at the magnetic field position of the main peak (341.5 mT). This echo decay immediately shows ESEEM during the initial time range.
Relaxation times T1 and T2 were calculated theoretically using the CW-ESR parameter. We used pulsed-ESR and CW-ESR to calculate T1 and T2. We revealed that T1 and T2 from pulsed-ESR and CW-ESR were changed similarly before and after irradiation.
We would like to extend our deepest gratitude to Prof. Anders Lund (Linko°ping University) and Prof. Sergei A. Dzuba (Institute of Chemical Kinetics and Combustion) for their valuable advice and guidance.
Liquid crystals investigation was begun by an Austrian scientist, Friedrich Reinitzer in 1888 when he espied a material named cholesteryl benzoate having two different melting points. He manipulated the temperature of the samples in his experiments and observed the changes that happened. Due to this early work, Reinitzer is attributed with the discovery of a new phase of matter - the liquid crystal phase and since then, liquid crystals have been under study for various research fields including physics, chemistry, medicine as well as engineering that resulted in the advanced nanostructured liquid crystals exhibiting an extraordinary ordered pattern and highlighting advanced functions such as electro-optical effects, chromism, sensing and templating [1, 2, 3].
The state of matter which shows liquid and crystalline properties at the same time is known as a liquid crystal, and this dual state of matter not only possesses viscous properties like fluidity, formation of droplets and mechanical properties but also exhibits the nature of crystalline solids such as periodic and anisotropic properties; therefore, they are named mesophases [4]. Liquid crystals are gaining popularity due to their remarkable functional properties, due to their ability to respond to external stimuli such as heat, light, electric fields, and mechanical forces [5]. Liquid phase molecules have no defined intrinsic order, while solid molecules are highly ordered, and the distinguishing property of liquid crystal is the inclination of molecules to point along the same direction of axis, called an anisotropic property [6] as shown in Figure 1 [7]. Liquid crystals are classified into two primary groups based on various conditions and parameters: thermotropic and lyotropic liquid crystals, which differ in their arrangement mechanism but share many properties.
A comparison of solid, liquid and liquid crystal orientation [
Thermotropic liquid crystals may be created by heating crystalline structures, which causes molecular position order to disappear but not the molecular orientational order, resulting in a dynamic phase with anisotropic liquid crystal characteristics [8]. This type of liquid crystal is temperature-dependent, with high temperatures resulting in an ordinary isotropic liquid phase owing to disrupted phase ordering, and low temperatures resulting in an anisotropic ordered crystalline liquid phase. On the other hand, an organized structure in a colloidal solution creates lyotropic liquid crystals that are formed by amphiphilic molecules with hydrophilic and hydrophobic portions. By changing the concentration and temperature of amphiphilic molecules, different lyotropic phases may be produced [9].
Liquid crystal classifications on an extensive level open up ways for various fundamental meso-phases. The chemical and physical properties of liquid crystals vary by changing temperature, solution concentration and other parameters that resulted in long-range orientational as well as positional order of molecules. Thermotropic liquid crystals result in different kinds of meso-phases due to varying temperatures, and these transactions are controlled thermally. The mechanism further divides thermotropic liquid crystals into two categories: enantiotropic liquid crystals, which can be obtained by only decreasing the liquid temperature or increasing the solid temperature, and monotropic liquid crystals, which can be obtained by either increasing the temperature of a solid-state material or decreasing the temperature of a liquid state material to form an aligned as well as ordered liquid crystal arrangement. Depending on the molecular arrangement and symmetry, thermotropic liquid crystals are subdivided into four main categories; nematics, cholesterics, smectics, and columnar liquid crystals. The orientational order, positional order, and bond orientational order are some of the characteristics that describe liquid crystal formations. Nematic mesophase is the fundamental liquid crystal phase in which the molecular orientation is correlated with local molecular-axis orientation that can be controlled by external factors like; an electric field that helps the molecular axis to align accordingly [10], as is shown in Figure 2(a) [11]. These liquid crystal structures have a long-range orientational order but they lack in order of molecular center of mass positions, and are anisotropic having a rigid molecular backbone that outlines the long axis of molecules. Because they have a strong dipole moment and a high refractive index, these crystalline compounds may easily be polarized, making them useful in display applications [12].
(a) Nematic liquid crystal [
Cholesteric liquid crystal state is comparable to nematic state [13], having nematic layers where each layer has its director; therefore, it is known as the counterpart of the nematic phase, as is shown in Figure 2(b) [14]. Likewise, these compounds exhibit long-range orientational order owing to their molecular organization into a long axis that is parallel to the molecular plan, and the molecular axis is defined as helical. The cholesteric structure is characterized by the pitch that is the distance along the long-axis on which the director rotates. Cholesterics are finite pitch structures with a few hundred nanometers of pitch; however, nematics can also be of the finite pitch if doped with an enantiomorphic compound. Cholesteric structure pitch is comparable to visible light, resulting in white light scattering owing to Bragg’s reflection phenomenon, which may be exploited for different optical applications although this pitch can also be sensitive to numerous variables [15, 16, 17].
Smectic liquid crystals differ from others owing to layer ordering but molecule orientation is comparable to nematic in addition to layer alignment, and these structures have both positional and orientational orders. The smectic liquid crystal phases exhibit molecules organized perpendicular to layers, hexagonally structured, and tilt angle measurement in smectic types A, B, and C; however, they are more ordered than the nematic liquid crystal phases. Figure 3 depicts smectic A and C with no molecular positional ordered inside each individual layer, where smectic A molecules are orientated perpendicular along with the layer, but smectic C molecules are tilted away from the layer orientation, and so have order in one direction only.
Smectic A, Smectic C liquid crystal schematic diagram [
Columnar liquid crystals are also known as discotic liquid crystals due to the disc-shaped molecular structures that are stacked in column form and organized in various shapes [18], while the columnar phase molecules are classified based on their packing motivations. They are arranged in 2D patterns such as hexagonal, rectangular, oblique, and lamellar [19] and these molecules are stacked in their respective lattices as shown in Figure 4.
Columnar phase liquid crystals schematic diagram; (a) hexagonal, (b) rectangle, (c) oblique, and (d) lamellar [
Another classification of liquid crystal, lyotropic liquid crystal transitions, occurred by changing solvent concentration as well as varying the temperature. Amphiphilic molecules in a solution with hydrophobic and hydrophilic components resulted in diverse lyotropic liquid crystals and varied concentrations resulted in various circular or rod-shaped micelles in a solution. The rod-shaped micelles are arranged to form highly viscous hexagonal lyotropic liquid crystal while the circular micelle form a cubic pattern of lyotropic liquid crystal that does not have shear planes to make them more viscous than the hexagonal lyotropic phase. Shape-dependent numerous kinds of lyotropic liquid crystals can be obtained by manipulating the micelle shape present in the solution [20, 21].
There have been relatively few computational approaches to the advancement of liquid crystals since their discovery. In the 1940s, Onsager showed the colloidal solution method for liquid crystal formation, and proved that transitions can be occurred from isotropic to anisotropic phase by changing the density [22]. Then, in the 1950s, Maier and Saupe developed the molecular mean-field theory that explained the temperature-dependent transitions of thermotropic liquid crystals [23]; however, in comparison to these theories, the first simulation theory linked to simple liquid crystals was developed in the 1990s [24]. In recent years, attempts have been made to investigate simulation approaches and methodologies for determining the functions and properties of liquid crystals. The most challenging aspect in molecular simulation is connecting different lengths as well as the time of action scales, and various models are employed to manage these simulations based on their time scales, as shown in Figure 5. Molecular bonds and intermolecular motions in the femto-second time scale range are addressed by quantum modeling, while atomistic modeling handles molecular bond motion to liquid crystal director alignment in the femto-to-nanosecond time scale. The coarse-grained approach facilitated simulations of liquid crystal polymers at nanosecond to microsecond time scales, whereas continuum modeling is better suited to simulations at longer length and time scales.
Computational schemes employed in liquid crystals research [
Quantum modeling mainly addressed the intermolecular motion with a time scale range of femto-seconds, whereas atomistic modeling is considered to be the vanguard of computational analysis of nanomaterials, and it plays a pivotal role as an interfacial region. The building complex models have also proven to be an effective tool for predicting the relationship between macroscopic properties and underlying atomistic structures. The structural analysis of a material is obtained at the end of molecular dynamics or Monte Carlo simulations, and it reflects the pair correlation function, which yields the probability of atomic separation by some calculated distance, and it can then be compared with experimental data to validate the computational as well as model methodology, ensuring that results correspond to the experimental setup. The coarse-grained models are vital for the illustration of complex systems that allow keeping the main entities and performing the important simulations that are not more suitable with other simulation methods like molecular dynamics having some limitations in time and length scales. The group of atoms is bounded by beads whose interaction depends on their internal energy function which accounts for the detailed simulations at the atomistic level for both bonded and non-bonded interactions. This modelling method can be applied to a wide range of length scales, such as a bead or interaction site of a group of atoms, a functional group, or a polymeric micro-particle, depending entirely on the system of interest and the investigated property [26].
Continuum models are proved as the most useful description of lateral composition segregation that measures the tendency of a solid solution to possess the phase separation. It has also been reported that continuum simulation is more feasible for more precise modeling of the mechanics problem of stress relaxation by lateral region formation of phase-separated material, where the system goes from constrained to less-stressed configuration and the tendency towards phase separation may decrease. The kinetics of morphological evolution reflects these transitions and is a superior alternative for simulations with larger lengths and time scales [27]. Molecular modeling becomes difficult as the length and time scales increase, thus various sophisticated simulation techniques are employed, including lattice Boltzmann nemato-dynamics [28], reduction of the Landau-de Gennes free energy [29], and continuum theory approaches [30]. The liquid crystal force field method is appropriate for a wide range of molecular stands. Bond stretching, bond bending, and torsional potential may be calculated using ab-initio / DFT [31] calculations and the force field approach in combination with sophisticated computer technology.
The recent advancements in computer simulation of liquid crystals classified them into three main categories; hard non-spherical models, soft non-spherical models and lattice models.
The hard non-spherical model is based on the fact that liquid crystal molecules are generally non-spherical hard ellipsoids, and hard sphero-cylinders, as shown in Figure 6. This intriguing feature would be useful in studying the basic effects and assessing the liquid crystal stability as well as other external stimuli interactions, whereas the phase behavior of these hard molecule-based models is reliant on density changes and is independent of temperature. This feature of liquid crystal molecules is demonstrated by Onsager’s work [22], in which he deduced that transitions from isotropic to anisotropic occur well below the density at which the system would be expected to crystallize, provided that length is much greater than the diameter, and represent a non-spherical pattern. The interplay between translational and rotational entropy is the driving factor behind liquid crystal formation; as density increases the system minimizes its free energy by organizing itself, causing a rise in translational and rotational entropy.
Simulations of hard sphero-cylinders with aspect ratio L/D = 5 at different densities [
Non-spherical simulations were done in the 1970s and subsequent years, but due to a lack of computer time, these simulations were not completed properly [33, 34, 35]. The original work has recently been expanded by combining thermodynamic and dynamical characteristics to calculate the value of electrons for non-spherical (ellipsoids) molecules and adding boundary constraints to decrease surface effects [36], revealing spontaneous liquid crystal ordering by an even compression of the isotropic state beyond the thermodynamic stable limit. However, using the molecular dynamic approach, it was discovered that the smectic phase develops from the nematic phase over time. This method allows for the comparison of diffusion coefficients parallel to smectic planes, which reveals mobility within layers and motion between layers in the perpendicular direction.
Liquid crystal molecules in a soft non-spherical model are soft and feature long-range molecular interactions, whereas temperature is used to determine thermodynamic equilibrium in this model, which was not studied in hard non-spherical models. The invention of the Gaussian overlap model [37] started work in this field in the 1970s, and the Gay-Berne potential is the most often used soft non-spherical model. This model, which was founded on the notion of fitting the potentials to a more exact atomic model of the molecule of interest [38], incorporates the attraction of soft ellipsoids, which have the same symmetry as hard ellipsoids. Although, the initial potential had unrealistic features, it has subsequently been improved and widely used [36]. The Gay-Berne (GB) model has the advantage of being able to explore a wide range of interactions between various thermotropic liquid crystals by adjusting the potential and well-depth parameters, as well as being simple to combine with other potentials. Recent results combine GB and a point dipole to illustrate the ferroelectric phase [39], as well as GB with a point quadrupole to demonstrate the smectic C phase [40]. Because this model includes a temperature factor, an isotropic phase was formed at high temperatures, but upon cooling, a nematic phase was observed, indicating that the smectic A phase was obtained, while further cooling yielded hexagonal alignment within the layers, indicating that the smectic B phase was obtained. Molecular diffusions can be identified as the temperature is reduced further [36], demonstrating that this advanced simulation model is capable of predicting thermodynamic transitions.
Lattice model has been popular in previous studies because of their simplicity and computational efficiency, such as the model shown in Figure 7, in which the chain stiffness is represented by a bond-bending efficiency that reduces the number of 90° lattice bends in some way. The most appealing feature of lattice model is that single-chain simulations may attain contour lengths of about 80,000 lattice spacing; nevertheless, the lack of small-angle bending deformations proposed by these models demonstrates the primary physical processes. Chains restricted by walls, for example, cannot show variations on the deflection length scale, but they can only show propagation along straight lines over lengths of the order of bond length (
Schematic representation of self-avoiding walk on a simple cubic lattice for the simulation of polymers [
Simulation and theoretical reasoning have recently demonstrated the feasibility of extrapolating from high-dimensional systems to three-dimensional systems in the real world [25]. Even the most basic Lebwohl-Lasher lattice model has the correct phase transition properties, which could be used to support Maier and Saupe’s original ideas that long-ranged, smoothly-varying interactions between ‘swarms’ of molecules are the most important factor in determining the stability of mesophases.
Liquid crystals have been considered peculiar substances since their discovery in 1888. The demand for low-power, high-efficiency displays invigorated research into liquid crystal electro-optical characteristics, and they offer a wide range of uses outside of displays, including switchable windows, thermometers, plasmonics, photovoltaics, and solar cells [43]. This section is devoted to exploring some useful and novel applications of LCs in different areas of day-to-day life as summarized in Table 1.
Potential application domains of liquid crystal research.
Graphene is an atomic-scale thin carbon material that has drawn much attention due to its unique and extraordinary electrical, chemical, thermal, mechanical and optoelectronic properties having a wide range of applications. Chemical oxidation of graphene produces graphene oxide, while wet chemical exfoliation of graphene produces graphene oxide-based liquid crystals [44]. Graphene oxide is unique in comparison to liquid crystal molecules because of its large diameter to thickness aspect ratio and optical anisotropy, exhibiting a strong magnetic response. Graphene oxide-based liquid crystals are employed in many display and device applications due to their electric field-induced birefringence. The devices based on graphene oxide consume less power than traditional liquid crystals and do not require specific electrode treatment. Also, the device size and switching time may be reduced by decreasing the size of the graphene oxide flakes [45]. When the size of the graphene oxide flakes decreases, the polarization anisotropy reduces quicker than the rotational viscosity, causing the rising time to increase, while falling time is controlled only by rotational viscosity, smaller flakes suffer less, resulting in a decrease in falling time, although, the smaller switching time is required for screen applications. Graphene oxide liquid crystals may also be utilized as rewritable boards with a dark or bright background [46], a reflective display that does not require polarizing optics and relies only on ambient light. These reflective displays which are controlled by an electric field are extensively used in electronic books because of their low energy consumption and inexpensive cost.
Liquid crystals have remarkable optical properties that respond to external stimuli such as light, temperature, electric field, magnetic field, and electrochemical reactions resulting in a dynamic change of material from the molecular to the macroscopic level, and this dynamic system makes them more useful in the nanofabrication of photonic materials. The responses of liquid crystals to various stimuli contribute to the photo bandgap tuneability, which has several uses in communication systems and optical integrated circuits. Photo crystals can control photons and hence offer a wide variety of uses based on defect engineering or the crystal bandgap; consequently, light can only be transmitted by adding defects, while the simultaneous introduction of point and line defects produces a miniature photonic circuit for different applications [47, 48, 49]. Photonic crystals may also influence light propagation through the structure resulting in a change in the propagation direction, slower propagation speed, and negative refraction. Controlled photonic devices are potential instruments for optical switching, routing, optical imaging, and power splitting because of their capabilities. This approach may also be employed to develop lasers with a narrow wavelength range on a tiny chip [50]. It is worth noting that, owing to better photonic crystal fabrication, 3D photonic crystals, rather than the currently utilized 2D crystals, will be used in future applications due to greater light control in the 3D range. Photonic crystal fibers can transmit a large range of light wavelengths with zero dispersion, and due to this uncommon property, they can be widely used for communication networks, polarization splitters, rotators, filters as well as multiplexers [43].
Liquid crystals are widely used in many photovoltaic devices owing to their unique intermolecular interactions. Discotic or columnar liquid crystals are more efficient to use and have more intermolecular interactions than inter-columnar interactions with special arrangements, in which each column acts as a molecular wire so that electrons and holes can move freely in one-dimensional structural arrangement and this alignment of molecules increases the electrical conductivity that allows them to be used in photovoltaic devices [51, 52]. Also, p-type and n-type discotic liquid crystals can be designed, and their properties, as well as alignment to the electrode surface, can be improved to achieve better charge migration results [53]. Calamitic or rod-like liquid crystals are also fascinating for semiconductor applications, particularly in display devices as well as conducting impurities [54]. In addition, liquid crystals create nanomorphology between the donor and acceptor layers to enhance film orientational order, resulting in efficient photocurrent generation and higher incoming photon conversion efficiency.
A newly emerging field that combines liquid crystals with nano-sized photonic structures is called nanophotonics [55], and is widely used in numerous applications. These devices are utilized to tune plasmonic nanostructures, as well as nanoporous materials, controlled magnetic field for switching liquid crystals and these liquid crystal composites with dielectric nanostructures are continuously gaining practical attention [56]. Liquid crystals are enabling to impart their long-ranged orientational symmetry to nanomaterials. Low concentrations of nanomaterials can be oriented as nematic patterns that can demonstrate improved physical properties of liquid crystals as well as a strong response to external stimuli such as electro-optic and magneto-optic responses, electrochemical memory effect, and changes in liquid crystal orientational order parameters [57]. Furthermore, the ability of liquid crystals to flow and fill nano-gaps led to the development of adjustable photonic crystal devices, porous silicon thermal tuning, and 2D photonic bandgap structures filled with liquid crystals [58]. Because nematic liquid crystals have poor magnetic anisotropy, switching the device requires a high magnetic field of about one Tesla, which would damage the device, so combining liquid crystals with ferromagnetic nanoparticles can be used to improve device switching at low magnetic fields for even better practical applications [59] that would result in some intriguing effects like increased dielectric anisotropy, increased order parameter as manifested by an increase in birefringence, enhanced non-linear effects, and so on, and these factors resulted in a decrease in threshold voltage, which is an important factor of power consumption in display applications [60].
Liquid crystals have gained much attention for plasmonic applications because of their attractive features such as; large birefringence, less driving threshold and various possible fabrication methods. This particular application of liquid crystals opens up the opportunities for next-generation plasmonic devices by combining both the liquid crystals and nanostructures with enhanced plasmonic properties resulted in devices such as; modulators, absorbers, plasmonic waveguides, plasmonic switches and color filters, etc. The main feature of liquid crystals that makes them suitable for active plasmonic devices is the difference in refractive index resulting in large birefringence. There are numerous ways to apply liquid crystals to the plasmonic nanostructures to get a promising change in refractive index that is essential for its potential device applications. Liquid crystal-based active plasmonic devices can be categorized according to the driving methods such as; electric field-driven method, heat-driven method, acoustic waves driven method and light-driven method. Depending on whether external biasing is supplied, such as an electric field, heat, light, or acoustic waves, liquid crystal molecules will align properly when exposed to external stimuli. This feature of liquid crystals is coupled with a periodic nanostructured material to produce the consequent controlled effect of plasmonic structures such as reflection, transmission, or absorption, indicating its potential in a variety of plasmonic-based devices [61]. Hence the combination of liquid crystals and metallic nanoparticles can be utilized to create tunable plasmonic devices, because metallic nanoparticles exhibit strong attenuation at resonance wavelengths that correspond to localized surface plasmon and this resonance wavelength can be modified by varying surrounding refractive index which can be controlled by external electric field using liquid crystals, yielding promising results [62, 63].
Since the previous decade, liquid crystals have been a popular issue, with considerable progress made in understanding their complicated process and alignments in many applications, particularly in display devices, which makes them fascinating. However, quite some important alignment aspects are not understood well specifically regarding liquid crystals molecular interactions, which is the biggest challenge in the liquid crystals industry of this era. There is a need for the developed alignment technology that would resolve the existing limiting factors that are affecting display quality and processing costs. The specific challenging areas of liquid crystals include non-uniform alignment over large displays, image sticking, uneven display brightness and multi-domain alignment pattern configurations [64]. Response time of liquid crystals is another challenge that plays an important role in display applications. Slow response time of liquid crystal causes blur quality and undesirable image display which is due to the non-adjustable pre-tilt angle of liquid crystals with the substrate that eventually affects the cell dynamics. To improve image quality and display, a proper oriented angle adjustment between liquid crystals and substrate is needed to be addressed [65]. Furthermore, anchoring energy, which is the energy necessary to deviate the director off the molecular axis at a specific angle, may be used to evaluate the alignment strength of the liquid crystal. Associated with the pre-tilt angle, stability of anchoring energy is another biggest challenge of liquid crystals industry to obtain uniform planer alignment, and to overcome this problem, rubbing mechanism was introduced to align liquid crystals, but this mechanism also faces challenges including static charge accumulation as well as dust-particle generation on crystal surface which affects the basic device characteristics and operational mechanism. The image sticking phenomena that happens when an image is shown for a long time is an essential aspect in determining the liquid crystal display quality. The present state of the problem of the liquid crystal [64] is indeed the electric charge or residual DC charge produced on the liquid crystal surface during long-term picture display, which causes selective surface adsorption of ionic impurities present in liquid crystal material or layers. Moreover, liquid crystals have some other drawbacks related to a huge number of ionic impurities present in aligned layers of liquid crystals and the presence of conjugated functional groups or lone pairs in liquid crystal molecules and between its aligned layers that would eventually result in disturbing as well as disrupting the display application, hence affecting the role of liquid crystals in device applications [66].
Liquid crystals are materials with extraordinary properties mainly because of the partial orientational order having application in electronic, display and non-display devices that have become a pervasive as well as unavoidable feature in routine life. The full exploration of these materials is still a challenge due to the tricky problems involved in its phase structures, and a wide range of thermotropic liquid crystals with different shapes are reported with molecular self-assembly and interactions. Despite molecular shape and properties, fascinating research trends highlights the lack of systematic studies. However, this gap can be considered for future research by developing standard techniques and procedures. In addition, the molecules can be modified by the functional units to obtain highly functional systems using a variety of unexplored solutions.
The progression in nanophotonics can be used in combination with liquid crystals to design tunable devices with the help of powerful computer simulations which would continue assisting the building and understanding of liquid crystal devices at atomistic as well as a molecular level. Because of developing nano-sized liquid crystals, the future decade is likely to reveal more novel adjustable technologies, and this area needs strong developments to generate models as well as techniques with enhanced phase behavior representation diagrams which would lead to study the structural changes along-with phase behavior to explore novel material properties. Polyphilic molecules, which provide various interaction regions in a molecule to incorporate other flexible materials, are another intriguing feature of liquid crystals, and they can be more beneficial by controlling the molecular self-assembly, which is the most difficult part of synthetic engineering. However, if simulations are sophisticated enough to be utilized as engineering tool to create polyphilic liquid crystals with the desired structures; the liquid crystal industry can achieve amazing success.
This chapter summarized an overview of liquid crystals by exploring fundamentals along with its recent computational advancement, challenges faced, applied applications and future prospects. Liquid crystals are unique in their properties having potential for numerous applied applications ranging from optical imaging, plasmonics, solar cells, photonic crystals, photovoltaics as well as nanophotonics, and the research in this field is the spark for the next forefront of economic development. Because of the combination of LCs with nanotechnology, the next decade will see noticeable developments and an increase in miniaturized tunable devices such as; tunable optical filters based on LCs and plasmonic phenomena like enhanced optical transmission through nano-slits, extinction of metallic nanoparticles and nanostructures, and LC biosensors that make use of LC and nanostructure characteristics.
IntechOpen - where academia and industry create content with global impact
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At this point, we relied on the firstly discovered ability of the DNA base mispairs to tautomerize via the sequential intrapair proton transfer and highly stable, highly polar, zwitterionic transition states, accompanied by a significant shifting of the base mispairs toward DNA minor or major grooves. These tautomeric transitions are characterized by a change in geometry—from wobble to Watson-Crick and vice versa—of the purine·pyrimidine (A·T, G·C, G·T and A·C), purine·purine (A·A, A·G and G·G) and pyrimidine·pyrimidine (С·С, С·T and Т·Т) DNA base mispairs. Reported results allow us to explain, on one side, the origin of the mutagenic tautomers at the separation of the DNA strands before replication and, on the other side, how DNA base mispairs adapt to enzymatically competent size in the tight recognition pocket of the high-fidelity DNA polymerase.",book:{id:"6684",slug:"mitochondrial-dna-new-insights",title:"Mitochondrial DNA",fullTitle:"Mitochondrial DNA - New Insights"},signatures:"Ol’ha O. Brovarets’ and Dmytro M. 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Al-Allaf",authors:[{id:"28112",title:"Dr.",name:"Oleg",middleName:"E",surname:"Tolmachov",slug:"oleg-tolmachov",fullName:"Oleg Tolmachov"},{id:"71555",title:"Dr.",name:"Faisal A.",middleName:null,surname:"Al-Allaf",slug:"faisal-a.-al-allaf",fullName:"Faisal A. Al-Allaf"},{id:"71556",title:"Dr.",name:"Tanya",middleName:null,surname:"Tolmachova",slug:"tanya-tolmachova",fullName:"Tanya Tolmachova"}]},{id:"22180",title:"The Role of DNA Repair Pathways in Adeno-Associated Virus Infection and Viral Genome Replication / Recombination / Integration",slug:"the-role-of-dna-repair-pathways-in-adeno-associated-virus-infection-and-viral-genome-replication-rec",totalDownloads:2477,totalCrossrefCites:3,totalDimensionsCites:3,abstract:null,book:{id:"1281",slug:"dna-repair-and-human-health",title:"DNA Repair and Human Health",fullTitle:"DNA Repair and Human Health"},signatures:"Kei Adachi and Hiroyuki Nakai",authors:[{id:"56392",title:"Dr.",name:"Hiroyuki",middleName:null,surname:"Nakai",slug:"hiroyuki-nakai",fullName:"Hiroyuki Nakai"},{id:"58003",title:"Dr.",name:"Kei",middleName:null,surname:"Adachi",slug:"kei-adachi",fullName:"Kei Adachi"}]},{id:"49580",title:"AAV Biology, Infectivity and Therapeutic Use from Bench to Clinic",slug:"aav-biology-infectivity-and-therapeutic-use-from-bench-to-clinic",totalDownloads:3258,totalCrossrefCites:12,totalDimensionsCites:18,abstract:"Adeno-associated virus (AAV) has been isolated from numerous vertebrate species since 1966. Besides its wide and promiscuous tropism, AAV infection does not result in considerable toxicity or pathogenicity and is capable of achieving adequate and long-term levels of gene transfer, especially following generation of the AAV recombinant variant: rAAV. Due to these properties, rAAV has gained special attention as a viral vector for gene therapy in the last decade. Currently, there are 130 clinical trials taking place worldwide for several diseases testing the safety and efficacy profiles of rAAV. During preclinical and clinical studies, several challenges have arisen in terms of reaching the full therapeutic potential of rAAV, such as efficient delivery of the virus in a targeted and specific manner to a desired tissue. Importantly, the development of immune responses towards the viral capsids poses an obstacle to rAAV applicability in the clinical setting. Numerous approaches have been developed in order to tailor an optimized therapeutic virus for treating specific diseases, including the use of different AAV serotypes or the creation of recombinant capsid variants with distinctive transduction and immunological profiles. This chapter reviews current information on rAAV clinical trials and the potential for combining rAAV platform with other technologies, such as induced pluripotent cells and gene editing.",book:{id:"4754",slug:"gene-therapy-principles-and-challenges",title:"Gene Therapy",fullTitle:"Gene Therapy - Principles and Challenges"},signatures:"Melisa A. Vance, Angela Mitchell and Richard J. Samulski",authors:[{id:"174649",title:"Ph.D.",name:"Melisa",middleName:null,surname:"Vance",slug:"melisa-vance",fullName:"Melisa Vance"},{id:"175144",title:"Dr.",name:"R. Jude",middleName:null,surname:"Samulski",slug:"r.-jude-samulski",fullName:"R. Jude Samulski"},{id:"178296",title:"Dr.",name:"Angela",middleName:null,surname:"Mitchell",slug:"angela-mitchell",fullName:"Angela Mitchell"}]},{id:"63034",title:"Mitochondrial Dysfunction Associated with Doxorubicin",slug:"mitochondrial-dysfunction-associated-with-doxorubicin",totalDownloads:1684,totalCrossrefCites:6,totalDimensionsCites:13,abstract:"Cancer prevalence is scaling up each year. Anthracycline groups are still the best chemotherapeutic agent. The most popular anticancer drug in the group is doxorubicin (DOX). Unfortunately, DOX has potent toxicity on noncancerous tissues, e.g., heart, kidneys, etc. However, it is well documented that the severest toxicity of the drug affects heart tissue. Of course, some reasons have been suggested why and/or how the heart is so vulnerable to toxicity. The primary mechanism responsible for DOX’s cardiospecific toxicity remains unidentified so far; however, mitochondrial dysfunction induced by DOX is now considered one of the leading reasons for DOX’s toxicities and undesired side effects. Mitochondrial reactive oxygen production in the heart is a significant contributor to developing mitochondrial dysfunction-exposed DOX based on a variety of evidence. The objective of this review chapter is to critically evaluate and highlight the role of mitochondria in the development of DOX-induced cardiotoxicity.",book:{id:"6060",slug:"mitochondrial-diseases",title:"Mitochondrial Diseases",fullTitle:"Mitochondrial Diseases"},signatures:"Celal Guven, Yusuf Sevgiler and Eylem Taskin",authors:[{id:"192567",title:"Prof.",name:"Eylem",middleName:null,surname:"Taskin",slug:"eylem-taskin",fullName:"Eylem Taskin"},{id:"195229",title:"Dr.",name:"Celal",middleName:null,surname:"Guven",slug:"celal-guven",fullName:"Celal Guven"},{id:"206996",title:"Prof.",name:"Yusuf",middleName:null,surname:"Sevgiler",slug:"yusuf-sevgiler",fullName:"Yusuf Sevgiler"}]}],onlineFirstChaptersFilter:{topicId:"186",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:3,numberOfUpcomingTopics:0,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:"11",title:"Biochemistry",doi:"10.5772/intechopen.72877",issn:"2632-0983",scope:"Biochemistry, the study of chemical transformations occurring within living organisms, impacts all areas of life sciences, from molecular crystallography and genetics to ecology, medicine, and population biology. Biochemistry examines macromolecules - proteins, nucleic acids, carbohydrates, and lipids – and their building blocks, structures, functions, and interactions. Much of biochemistry is devoted to enzymes, proteins that catalyze chemical reactions, enzyme structures, mechanisms of action and their roles within cells. Biochemistry also studies small signaling molecules, coenzymes, inhibitors, vitamins, and hormones, which play roles in life processes. Biochemical experimentation, besides coopting classical chemistry methods, e.g., chromatography, adopted new techniques, e.g., X-ray diffraction, electron microscopy, NMR, radioisotopes, and developed sophisticated microbial genetic tools, e.g., auxotroph mutants and their revertants, fermentation, etc. More recently, biochemistry embraced the ‘big data’ omics systems. Initial biochemical studies have been exclusively analytic: dissecting, purifying, and examining individual components of a biological system; in the apt words of Efraim Racker (1913 –1991), “Don’t waste clean thinking on dirty enzymes.” Today, however, biochemistry is becoming more agglomerative and comprehensive, setting out to integrate and describe entirely particular biological systems. The ‘big data’ metabolomics can define the complement of small molecules, e.g., in a soil or biofilm sample; proteomics can distinguish all the comprising proteins, e.g., serum; metagenomics can identify all the genes in a complex environment, e.g., the bovine rumen. This Biochemistry Series will address the current research on biomolecules and the emerging trends with great promise.",coverUrl:"https://cdn.intechopen.com/series/covers/11.jpg",latestPublicationDate:"June 29th, 2022",hasOnlineFirst:!0,numberOfPublishedBooks:32,editor:{id:"31610",title:"Dr.",name:"Miroslav",middleName:null,surname:"Blumenberg",slug:"miroslav-blumenberg",fullName:"Miroslav Blumenberg",profilePictureURL:"https://mts.intechopen.com/storage/users/31610/images/system/31610.jpg",biography:"Miroslav Blumenberg, Ph.D., was born in Subotica and received his BSc in Belgrade, Yugoslavia. He completed his Ph.D. at MIT in Organic Chemistry; he followed up his Ph.D. with two postdoctoral study periods at Stanford University. Since 1983, he has been a faculty member of the RO Perelman Department of Dermatology, NYU School of Medicine, where he is codirector of a training grant in cutaneous biology. Dr. Blumenberg’s research is focused on the epidermis, expression of keratin genes, transcription profiling, keratinocyte differentiation, inflammatory diseases and cancers, and most recently the effects of the microbiome on the skin. He has published more than 100 peer-reviewed research articles and graduated numerous Ph.D. and postdoctoral students.",institutionString:null,institution:{name:"New York University Langone Medical Center",institutionURL:null,country:{name:"United States of America"}}},editorTwo:null,editorThree:null},subseries:{paginationCount:4,paginationItems:[{id:"14",title:"Cell and Molecular Biology",coverUrl:"https://cdn.intechopen.com/series_topics/covers/14.jpg",isOpenForSubmission:!0,editor:{id:"165627",title:"Dr.",name:"Rosa María",middleName:null,surname:"Martínez-Espinosa",slug:"rosa-maria-martinez-espinosa",fullName:"Rosa María Martínez-Espinosa",profilePictureURL:"https://mts.intechopen.com/storage/users/165627/images/system/165627.jpeg",biography:"Dr. Rosa María Martínez-Espinosa has been a Spanish Full Professor since 2020 (Biochemistry and Molecular Biology) and is currently Vice-President of International Relations and Cooperation development and leader of the research group 'Applied Biochemistry” (University of Alicante, Spain). Other positions she has held at the university include Vice-Dean of Master Programs, Vice-Dean of the Degree in Biology and Vice-Dean for Mobility and Enterprise and Engagement at the Faculty of Science (University of Alicante). She received her Bachelor in Biology in 1998 (University of Alicante) and her PhD in 2003 (Biochemistry, University of Alicante). She undertook post-doctoral research at the University of East Anglia (Norwich, U.K. 2004-2005; 2007-2008).\nHer multidisciplinary research focuses on investigating archaea and their potential applications in biotechnology. She has an H-index of 21. She has authored one patent and has published more than 70 indexed papers and around 60 book chapters.\nShe has contributed to more than 150 national and international meetings during the last 15 years. Her research interests include archaea metabolism, enzymes purification and characterization, gene regulation, carotenoids and bioplastics production, antioxidant\ncompounds, waste water treatments, and brines bioremediation.\nRosa María’s other roles include editorial board member for several journals related\nto biochemistry, reviewer for more than 60 journals (biochemistry, molecular biology, biotechnology, chemistry and microbiology) and president of several organizing committees in international meetings related to the N-cycle or respiratory processes.",institutionString:null,institution:{name:"University of Alicante",institutionURL:null,country:{name:"Spain"}}},editorTwo:null,editorThree:null},{id:"15",title:"Chemical Biology",coverUrl:"https://cdn.intechopen.com/series_topics/covers/15.jpg",isOpenForSubmission:!0,editor:{id:"441442",title:"Dr.",name:"Şükrü",middleName:null,surname:"Beydemir",slug:"sukru-beydemir",fullName:"Şükrü Beydemir",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0033Y00003GsUoIQAV/Profile_Picture_1634557147521",biography:"Dr. Şükrü Beydemir obtained a BSc in Chemistry in 1995 from Yüzüncü Yıl University, MSc in Biochemistry in 1998, and PhD in Biochemistry in 2002 from Atatürk University, Turkey. He performed post-doctoral studies at Max-Planck Institute, Germany, and University of Florence, Italy in addition to making several scientific visits abroad. He currently works as a Full Professor of Biochemistry in the Faculty of Pharmacy, Anadolu University, Turkey. Dr. Beydemir has published over a hundred scientific papers spanning protein biochemistry, enzymology and medicinal chemistry, reviews, book chapters and presented several conferences to scientists worldwide. He has received numerous publication awards from various international scientific councils. He serves in the Editorial Board of several international journals. Dr. Beydemir is also Rector of Bilecik Şeyh Edebali University, Turkey.",institutionString:null,institution:{name:"Anadolu University",institutionURL:null,country:{name:"Turkey"}}},editorTwo:{id:"13652",title:"Prof.",name:"Deniz",middleName:null,surname:"Ekinci",slug:"deniz-ekinci",fullName:"Deniz Ekinci",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002aYLT1QAO/Profile_Picture_1634557223079",biography:"Dr. Deniz Ekinci obtained a BSc in Chemistry in 2004, MSc in Biochemistry in 2006, and PhD in Biochemistry in 2009 from Atatürk University, Turkey. He studied at Stetson University, USA, in 2007-2008 and at the Max Planck Institute of Molecular Cell Biology and Genetics, Germany, in 2009-2010. Dr. Ekinci currently works as a Full Professor of Biochemistry in the Faculty of Agriculture and is the Head of the Enzyme and Microbial Biotechnology Division, Ondokuz Mayıs University, Turkey. He is a member of the Turkish Biochemical Society, American Chemical Society, and German Genetics society. Dr. Ekinci published around ninety scientific papers, reviews and book chapters, and presented several conferences to scientists. He has received numerous publication awards from several scientific councils. Dr. Ekinci serves as the Editor in Chief of four international books and is involved in the Editorial Board of several international journals.",institutionString:null,institution:{name:"Ondokuz Mayıs University",institutionURL:null,country:{name:"Turkey"}}},editorThree:null},{id:"17",title:"Metabolism",coverUrl:"https://cdn.intechopen.com/series_topics/covers/17.jpg",isOpenForSubmission:!0,editor:{id:"138626",title:"Dr.",name:"Yannis",middleName:null,surname:"Karamanos",slug:"yannis-karamanos",fullName:"Yannis Karamanos",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002g6Jv2QAE/Profile_Picture_1629356660984",biography:"Yannis Karamanos, born in Greece in 1953, completed his pre-graduate studies at the Université Pierre et Marie Curie, Paris, then his Masters and Doctoral degree at the Université de Lille (1983). He was associate professor at the University of Limoges (1987) before becoming full professor of biochemistry at the Université d’Artois (1996). He worked on the structure-function relationships of glycoconjugates and his main project was the investigations on the biological roles of the de-N-glycosylation enzymes (Endo-N-acetyl-β-D-glucosaminidase and peptide-N4-(N-acetyl-β-glucosaminyl) asparagine amidase). From 2002 he contributes to the understanding of the Blood-brain barrier functioning using proteomics approaches. He has published more than 70 papers. His teaching areas are energy metabolism and regulation, integration and organ specialization and metabolic adaptation.",institutionString:null,institution:{name:"Artois University",institutionURL:null,country:{name:"France"}}},editorTwo:null,editorThree:null},{id:"18",title:"Proteomics",coverUrl:"https://cdn.intechopen.com/series_topics/covers/18.jpg",isOpenForSubmission:!0,editor:{id:"200689",title:"Prof.",name:"Paolo",middleName:null,surname:"Iadarola",slug:"paolo-iadarola",fullName:"Paolo Iadarola",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bSCl8QAG/Profile_Picture_1623568118342",biography:"Paolo Iadarola graduated with a degree in Chemistry from the University of Pavia (Italy) in July 1972. He then worked as an Assistant Professor at the Faculty of Science of the same University until 1984. In 1985, Prof. Iadarola became Associate Professor at the Department of Biology and Biotechnologies of the University of Pavia and retired in October 2017. Since then, he has been working as an Adjunct Professor in the same Department at the University of Pavia. His research activity during the first years was primarily focused on the purification and structural characterization of enzymes from animal and plant sources. During this period, Prof. Iadarola familiarized himself with the conventional techniques used in column chromatography, spectrophotometry, manual Edman degradation, and electrophoresis). Since 1995, he has been working on: i) the determination in biological fluids (serum, urine, bronchoalveolar lavage, sputum) of proteolytic activities involved in the degradation processes of connective tissue matrix, and ii) on the identification of biological markers of lung diseases. In this context, he has developed and validated new methodologies (e.g., Capillary Electrophoresis coupled to Laser-Induced Fluorescence, CE-LIF) whose application enabled him to determine both the amounts of biochemical markers (Desmosines) in urine/serum of patients affected by Chronic Obstructive Pulmonary Disease (COPD) and the activity of proteolytic enzymes (Human Neutrophil Elastase, Cathepsin G, Pseudomonas aeruginosa elastase) in sputa of these patients. More recently, Prof. Iadarola was involved in developing techniques such as two-dimensional electrophoresis coupled to liquid chromatography/mass spectrometry (2DE-LC/MS) for the proteomic analysis of biological fluids aimed at the identification of potential biomarkers of different lung diseases. He is the author of about 150 publications (According to Scopus: H-Index: 23; Total citations: 1568- According to WOS: H-Index: 20; Total Citations: 1296) of peer-reviewed international journals. He is a Consultant Reviewer for several journals, including the Journal of Chromatography A, Journal of Chromatography B, Plos ONE, Proteomes, International Journal of Molecular Science, Biotech, Electrophoresis, and others. He is also Associate Editor of Biotech.",institutionString:null,institution:{name:"University of Pavia",institutionURL:null,country:{name:"Italy"}}},editorTwo:{id:"201414",title:"Dr.",name:"Simona",middleName:null,surname:"Viglio",slug:"simona-viglio",fullName:"Simona Viglio",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bRKDHQA4/Profile_Picture_1630402531487",biography:"Simona Viglio is an Associate Professor of Biochemistry at the Department of Molecular Medicine at the University of Pavia. She has been working since 1995 on the determination of proteolytic enzymes involved in the degradation process of connective tissue matrix and on the identification of biological markers of lung diseases. She gained considerable experience in developing and validating new methodologies whose applications allowed her to determine both the amount of biomarkers (Desmosine and Isodesmosine) in the urine of patients affected by COPD, and the activity of proteolytic enzymes (HNE, Cathepsin G, Pseudomonas aeruginosa elastase) in the sputa of these patients. Simona Viglio was also involved in research dealing with the supplementation of amino acids in patients with brain injury and chronic heart failure. She is presently engaged in the development of 2-DE and LC-MS techniques for the study of proteomics in biological fluids. The aim of this research is the identification of potential biomarkers of lung diseases. She is an author of about 90 publications (According to Scopus: H-Index: 23; According to WOS: H-Index: 20) on peer-reviewed journals, a member of the “Società Italiana di Biochimica e Biologia Molecolare,“ and a Consultant Reviewer for International Journal of Molecular Science, Journal of Chromatography A, COPD, Plos ONE and Nutritional Neuroscience.",institutionString:null,institution:{name:"University of Pavia",institutionURL:null,country:{name:"Italy"}}},editorThree:null}]},overviewPageOFChapters:{paginationCount:36,paginationItems:[{id:"82195",title:"Endoplasmic Reticulum: A Hub in Lipid Homeostasis",doi:"10.5772/intechopen.105450",signatures:"Raúl Ventura and María Isabel Hernández-Alvarez",slug:"endoplasmic-reticulum-a-hub-in-lipid-homeostasis",totalDownloads:3,totalCrossrefCites:0,totalDimensionsCites:0,authors:null,book:{title:"Updates on Endoplasmic Reticulum",coverURL:"https://cdn.intechopen.com/books/images_new/11674.jpg",subseries:{id:"14",title:"Cell and Molecular Biology"}}},{id:"82409",title:"Purinergic Signaling in Covid-19 Disease",doi:"10.5772/intechopen.105008",signatures:"Hailian Shen",slug:"purinergic-signaling-in-covid-19-disease",totalDownloads:3,totalCrossrefCites:0,totalDimensionsCites:0,authors:null,book:{title:"Purinergic System",coverURL:"https://cdn.intechopen.com/books/images_new/10801.jpg",subseries:{id:"17",title:"Metabolism"}}},{id:"82374",title:"The Potential of the Purinergic System as a Therapeutic Target of Natural Compounds in Cutaneous Melanoma",doi:"10.5772/intechopen.105457",signatures:"Gilnei Bruno da Silva, Daiane Manica, Marcelo Moreno and Margarete Dulce Bagatini",slug:"the-potential-of-the-purinergic-system-as-a-therapeutic-target-of-natural-compounds-in-cutaneous-mel",totalDownloads:9,totalCrossrefCites:0,totalDimensionsCites:0,authors:null,book:{title:"Purinergic System",coverURL:"https://cdn.intechopen.com/books/images_new/10801.jpg",subseries:{id:"17",title:"Metabolism"}}},{id:"82103",title:"The Role of Endoplasmic Reticulum Stress and Its Regulation in the Progression of Neurological and Infectious Diseases",doi:"10.5772/intechopen.105543",signatures:"Mary Dover, Michael Kishek, Miranda Eddins, Naneeta Desar, Ketema Paul and Milan Fiala",slug:"the-role-of-endoplasmic-reticulum-stress-and-its-regulation-in-the-progression-of-neurological-and-i",totalDownloads:6,totalCrossrefCites:0,totalDimensionsCites:0,authors:null,book:{title:"Updates on Endoplasmic Reticulum",coverURL:"https://cdn.intechopen.com/books/images_new/11674.jpg",subseries:{id:"14",title:"Cell and Molecular Biology"}}}]},overviewPagePublishedBooks:{paginationCount:32,paginationItems:[{type:"book",id:"7006",title:"Biochemistry and Health Benefits of Fatty Acids",subtitle:null,coverURL:"https://cdn.intechopen.com/books/images_new/7006.jpg",slug:"biochemistry-and-health-benefits-of-fatty-acids",publishedDate:"December 19th 2018",editedByType:"Edited by",bookSignature:"Viduranga Waisundara",hash:"c93a00abd68b5eba67e5e719f67fd20b",volumeInSeries:1,fullTitle:"Biochemistry and Health Benefits of Fatty Acids",editors:[{id:"194281",title:"Dr.",name:"Viduranga Y.",middleName:null,surname:"Waisundara",slug:"viduranga-y.-waisundara",fullName:"Viduranga Y. 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Singh",profilePictureURL:"https://mts.intechopen.com/storage/users/329385/images/system/329385.png",institutionString:"Punjab Technical University",institution:{name:"Punjab Technical University",institutionURL:null,country:{name:"India"}}}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null},{type:"book",id:"8018",title:"Extracellular Matrix",subtitle:"Developments and Therapeutics",coverURL:"https://cdn.intechopen.com/books/images_new/8018.jpg",slug:"extracellular-matrix-developments-and-therapeutics",publishedDate:"October 27th 2021",editedByType:"Edited by",bookSignature:"Rama Sashank Madhurapantula, Joseph Orgel P.R.O. and Zvi Loewy",hash:"c85e82851e80b40282ff9be99ddf2046",volumeInSeries:23,fullTitle:"Extracellular Matrix - Developments and Therapeutics",editors:[{id:"212416",title:"Dr.",name:"Rama Sashank",middleName:null,surname:"Madhurapantula",slug:"rama-sashank-madhurapantula",fullName:"Rama Sashank Madhurapantula",profilePictureURL:"https://mts.intechopen.com/storage/users/212416/images/system/212416.jpg",institutionString:"Illinois Institute of Technology",institution:{name:"Illinois Institute of Technology",institutionURL:null,country:{name:"United States of America"}}}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null},{type:"book",id:"9759",title:"Vitamin E in Health and Disease",subtitle:"Interactions, Diseases and Health Aspects",coverURL:"https://cdn.intechopen.com/books/images_new/9759.jpg",slug:"vitamin-e-in-health-and-disease-interactions-diseases-and-health-aspects",publishedDate:"October 6th 2021",editedByType:"Edited by",bookSignature:"Pınar Erkekoglu and Júlia Scherer Santos",hash:"6c3ddcc13626110de289b57f2516ac8f",volumeInSeries:22,fullTitle:"Vitamin E in Health and Disease - Interactions, Diseases and Health Aspects",editors:[{id:"109978",title:"Prof.",name:"Pınar",middleName:null,surname:"Erkekoğlu",slug:"pinar-erkekoglu",fullName:"Pınar Erkekoğlu",profilePictureURL:"https://mts.intechopen.com/storage/users/109978/images/system/109978.jpg",institutionString:"Hacettepe University",institution:{name:"Hacettepe University",institutionURL:null,country:{name:"Turkey"}}}],equalEditorOne:null,equalEditorTwo:null,equalEditorThree:null}]},subseriesFiltersForPublishedBooks:[{group:"subseries",caption:"Proteomics",value:18,count:4},{group:"subseries",caption:"Metabolism",value:17,count:6},{group:"subseries",caption:"Cell and Molecular Biology",value:14,count:9},{group:"subseries",caption:"Chemical Biology",value:15,count:13}],publicationYearFilters:[{group:"publicationYear",caption:"2022",value:2022,count:8},{group:"publicationYear",caption:"2021",value:2021,count:7},{group:"publicationYear",caption:"2020",value:2020,count:12},{group:"publicationYear",caption:"2019",value:2019,count:3},{group:"publicationYear",caption:"2018",value:2018,count:2}],authors:{paginationCount:229,paginationItems:[{id:"318170",title:"Dr.",name:"Aneesa",middleName:null,surname:"Moolla",slug:"aneesa-moolla",fullName:"Aneesa Moolla",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/318170/images/system/318170.png",biography:"Dr. Aneesa Moolla has extensive experience in the diverse fields of health care having previously worked in dental private practice, at the Red Cross Flying Doctors association, and in healthcare corporate settings. She is now a lecturer at the University of Witwatersrand, South Africa, and a principal researcher at the Health Economics and Epidemiology Research Office (HE2RO), South Africa. Dr. Moolla holds a Ph.D. in Psychology with her research being focused on mental health and resilience. In her professional work capacity, her research has further expanded into the fields of early childhood development, mental health, the HIV and TB care cascades, as well as COVID. She is also a UNESCO-trained International Bioethics Facilitator.",institutionString:"University of the Witwatersrand",institution:{name:"University of the Witwatersrand",country:{name:"South Africa"}}},{id:"419588",title:"Ph.D.",name:"Sergio",middleName:"Alexandre",surname:"Gehrke",slug:"sergio-gehrke",fullName:"Sergio Gehrke",position:null,profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0033Y000038WgMKQA0/Profile_Picture_2022-06-02T11:44:20.jpg",biography:"Dr. Sergio Alexandre Gehrke is a doctorate holder in two fields. The first is a Ph.D. in Cellular and Molecular Biology from the Pontificia Catholic University, Porto Alegre, Brazil, in 2010 and the other is an International Ph.D. in Bioengineering from the Universidad Miguel Hernandez, Elche/Alicante, Spain, obtained in 2020. In 2018, he completed a postdoctoral fellowship in Materials Engineering in the NUCLEMAT of the Pontificia Catholic University, Porto Alegre, Brazil. He is currently the Director of the Postgraduate Program in Implantology of the Bioface/UCAM/PgO (Montevideo, Uruguay), Director of the Cathedra of Biotechnology of the Catholic University of Murcia (Murcia, Spain), an Extraordinary Full Professor of the Catholic University of Murcia (Murcia, Spain) as well as the Director of the private center of research Biotecnos – Technology and Science (Montevideo, Uruguay). Applied biomaterials, cellular and molecular biology, and dental implants are among his research interests. He has published several original papers in renowned journals. In addition, he is also a Collaborating Professor in several Postgraduate programs at different universities all over the world.",institutionString:null,institution:{name:"Universidad Católica San Antonio de Murcia",country:{name:"Spain"}}},{id:"342152",title:"Dr.",name:"Santo",middleName:null,surname:"Grace Umesh",slug:"santo-grace-umesh",fullName:"Santo Grace Umesh",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/342152/images/16311_n.jpg",biography:null,institutionString:null,institution:{name:"SRM Dental College",country:{name:"India"}}},{id:"333647",title:"Dr.",name:"Shreya",middleName:null,surname:"Kishore",slug:"shreya-kishore",fullName:"Shreya Kishore",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/333647/images/14701_n.jpg",biography:"Dr. Shreya Kishore completed her Bachelor in Dental Surgery in Chettinad Dental College and Research Institute, Chennai, and her Master of Dental Surgery (Orthodontics) in Saveetha Dental College, Chennai. She is also Invisalign certified. She’s working as a Senior Lecturer in the Department of Orthodontics, SRM Dental College since November 2019. She is actively involved in teaching orthodontics to the undergraduates and the postgraduates. Her clinical research topics include new orthodontic brackets, fixed appliances and TADs. She’s published 4 articles in well renowned indexed journals and has a published patency of her own. Her private practice is currently limited to orthodontics and works as a consultant in various clinics.",institutionString:null,institution:{name:"SRM Dental College",country:{name:"India"}}},{id:"323731",title:"Prof.",name:"Deepak M.",middleName:"Macchindra",surname:"Vikhe",slug:"deepak-m.-vikhe",fullName:"Deepak M. Vikhe",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/323731/images/13613_n.jpg",biography:"Dr Deepak M.Vikhe .\n\n\t\n\tDr Deepak M.Vikhe , completed his Masters & PhD in Prosthodontics from Rural Dental College, Loni securing third rank in the Pravara Institute of Medical Sciences Deemed University. He was awarded Dr.G.C.DAS Memorial Award for Research on Implants at 39th IPS conference Dubai (U A E).He has two patents under his name. He has received Dr.Saraswati medal award for best research for implant study in 2017.He has received Fully funded scholarship to Spain ,university of Santiago de Compostela. He has completed fellowship in Implantlogy from Noble Biocare. \nHe has attended various conferences and CDE programmes and has national publications to his credit. His field of interest is in Implant supported prosthesis. Presently he is working as a associate professor in the Dept of Prosthodontics, Rural Dental College, Loni and maintains a successful private practice specialising in Implantology at Rahata.\n\nEmail: drdeepak_mvikhe@yahoo.com..................",institutionString:null,institution:{name:"Pravara Institute of Medical Sciences",country:{name:"India"}}},{id:"204110",title:"Dr.",name:"Ahmed A.",middleName:null,surname:"Madfa",slug:"ahmed-a.-madfa",fullName:"Ahmed A. Madfa",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/204110/images/system/204110.jpg",biography:"Dr. Madfa is currently Associate Professor of Endodontics at Thamar University and a visiting lecturer at Sana'a University and University of Sciences and Technology. He has more than 6 years of experience in teaching. His research interests include root canal morphology, functionally graded concept, dental biomaterials, epidemiology and dental education, biomimetic restoration, finite element analysis and endodontic regeneration. Dr. Madfa has numerous international publications, full articles, two patents, a book and a book chapter. Furthermore, he won 14 international scientific awards. Furthermore, he is involved in many academic activities ranging from editorial board member, reviewer for many international journals and postgraduate students' supervisor. Besides, I deliver many courses and training workshops at various scientific events. Dr. Madfa also regularly attends international conferences and holds administrative positions (Deputy Dean of the Faculty for Students’ & Academic Affairs and Deputy Head of Research Unit).",institutionString:"Thamar University",institution:null},{id:"210472",title:"Dr.",name:"Nermin",middleName:"Mohammed Ahmed",surname:"Yussif",slug:"nermin-yussif",fullName:"Nermin Yussif",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/210472/images/system/210472.jpg",biography:"Dr. Nermin Mohammed Ahmed Yussif is working at the Faculty of dentistry, University for October university for modern sciences and arts (MSA). Her areas of expertise include: periodontology, dental laserology, oral implantology, periodontal plastic surgeries, oral mesotherapy, nutrition, dental pharmacology. She is an editor and reviewer in numerous international journals.",institutionString:"MSA University",institution:null},{id:"204606",title:"Dr.",name:"Serdar",middleName:null,surname:"Gözler",slug:"serdar-gozler",fullName:"Serdar Gözler",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/204606/images/system/204606.jpeg",biography:"Dr. Serdar Gözler has completed his undergraduate studies at the Marmara University Faculty of Dentistry in 1978, followed by an assistantship in the Prosthesis Department of Dicle University Faculty of Dentistry. Starting his PhD work on non-resilient overdentures with Assoc. Prof. Hüsnü Yavuzyılmaz, he continued his studies with Prof. Dr. Gürbüz Öztürk of Istanbul University Faculty of Dentistry Department of Prosthodontics, this time on Gnatology. He attended training programs on occlusion, neurology, neurophysiology, EMG, radiology and biostatistics. In 1982, he presented his PhD thesis \\Gerber and Lauritzen Occlusion Analysis Techniques: Diagnosis Values,\\ at Istanbul University School of Dentistry, Department of Prosthodontics. As he was also working with Prof. Senih Çalıkkocaoğlu on The Physiology of Chewing at the same time, Gözler has written a chapter in Çalıkkocaoğlu\\'s book \\Complete Prostheses\\ entitled \\The Place of Neuromuscular Mechanism in Prosthetic Dentistry.\\ The book was published five times since by the Istanbul University Publications. Having presented in various conferences about occlusion analysis until 1998, Dr. Gözler has also decided to use the T-Scan II occlusion analysis method. Having been personally trained by Dr. Robert Kerstein on this method, Dr. Gözler has been lecturing on the T-Scan Occlusion Analysis Method in conferences both in Turkey and abroad. Dr. Gözler has various articles and presentations on Digital Occlusion Analysis methods. He is now Head of the TMD Clinic at Prosthodontic Department of Faculty of Dentistry , Istanbul Aydın University , Turkey.",institutionString:"Istanbul Aydin University",institution:{name:"Istanbul Aydın University",country:{name:"Turkey"}}},{id:"240870",title:"Ph.D.",name:"Alaa Eddin Omar",middleName:null,surname:"Al Ostwani",slug:"alaa-eddin-omar-al-ostwani",fullName:"Alaa Eddin Omar Al Ostwani",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/240870/images/system/240870.jpeg",biography:"Dr. Al Ostwani Alaa Eddin Omar received his Master in dentistry from Damascus University in 2010, and his Ph.D. in Pediatric Dentistry from Damascus University in 2014. Dr. Al Ostwani is an assistant professor and faculty member at IUST University since 2014. \nDuring his academic experience, he has received several awards including the scientific research award from the Union of Arab Universities, the Syrian gold medal and the international gold medal for invention and creativity. Dr. Al Ostwani is a Member of the International Association of Dental Traumatology and the Syrian Society for Research and Preventive Dentistry since 2017. He is also a Member of the Reviewer Board of International Journal of Dental Medicine (IJDM), and the Indian Journal of Conservative and Endodontics since 2016.",institutionString:"International University for Science and Technology.",institution:{name:"Islamic University of Science and Technology",country:{name:"India"}}},{id:"42847",title:"Dr.",name:"Belma",middleName:null,surname:"Işik Aslan",slug:"belma-isik-aslan",fullName:"Belma Işik Aslan",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/42847/images/system/42847.jpg",biography:"Dr. Belma IşIk Aslan was born in 1976 in Ankara-TURKEY. After graduating from TED Ankara College in 1994, she attended to Gazi University, Faculty of Dentistry in Ankara. She completed her PhD in orthodontic education at Gazi University between 1999-2005. Dr. Işık Aslan stayed at the Providence Hospital Craniofacial Institude and Reconstructive Surgery in Michigan, USA for three months as an observer. She worked as a specialist doctor at Gazi University, Dentistry Faculty, Department of Orthodontics between 2005-2014. She was appointed as associate professor in January, 2014 and as professor in 2021. Dr. Işık Aslan still works as an instructor at the same faculty. She has published a total of 35 articles, 10 book chapters, 39 conference proceedings both internationally and nationally. Also she was the academic editor of the international book 'Current Advances in Orthodontics'. She is a member of the Turkish Orthodontic Society and Turkish Cleft Lip and Palate Society. She is married and has 2 children. Her knowledge of English is at an advanced level.",institutionString:"Gazi University Dentistry Faculty Department of Orthodontics",institution:null},{id:"178412",title:"Associate Prof.",name:"Guhan",middleName:null,surname:"Dergin",slug:"guhan-dergin",fullName:"Guhan Dergin",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/178412/images/6954_n.jpg",biography:"Assoc. Prof. Dr. Gühan Dergin was born in 1973 in Izmit. He graduated from Marmara University Faculty of Dentistry in 1999. He completed his specialty of OMFS surgery in Marmara University Faculty of Dentistry and obtained his PhD degree in 2006. In 2005, he was invited as a visiting doctor in the Oral and Maxillofacial Surgery Department of the University of North Carolina, USA, where he went on a scholarship. Dr. Dergin still continues his academic career as an associate professor in Marmara University Faculty of Dentistry. He has many articles in international and national scientific journals and chapters in books.",institutionString:null,institution:{name:"Marmara University",country:{name:"Turkey"}}},{id:"178414",title:"Prof.",name:"Yusuf",middleName:null,surname:"Emes",slug:"yusuf-emes",fullName:"Yusuf Emes",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/178414/images/6953_n.jpg",biography:"Born in Istanbul in 1974, Dr. Emes graduated from Istanbul University Faculty of Dentistry in 1997 and completed his PhD degree in Istanbul University faculty of Dentistry Department of Oral and Maxillofacial Surgery in 2005. He has papers published in international and national scientific journals, including research articles on implantology, oroantral fistulas, odontogenic cysts, and temporomandibular disorders. Dr. Emes is currently working as a full-time academic staff in Istanbul University faculty of Dentistry Department of Oral and Maxillofacial Surgery.",institutionString:null,institution:{name:"Istanbul University",country:{name:"Turkey"}}},{id:"192229",title:"Ph.D.",name:"Ana Luiza",middleName:null,surname:"De Carvalho Felippini",slug:"ana-luiza-de-carvalho-felippini",fullName:"Ana Luiza De Carvalho Felippini",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/192229/images/system/192229.jpg",biography:null,institutionString:"University of São Paulo",institution:{name:"University of Sao Paulo",country:{name:"Brazil"}}},{id:"256851",title:"Prof.",name:"Ayşe",middleName:null,surname:"Gülşen",slug:"ayse-gulsen",fullName:"Ayşe Gülşen",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/256851/images/9696_n.jpg",biography:"Dr. Ayşe Gülşen graduated in 1990 from Faculty of Dentistry, University of Ankara and did a postgraduate program at University of Gazi. \nShe worked as an observer and research assistant in Craniofacial Surgery Departments in New York, Providence Hospital in Michigan and Chang Gung Memorial Hospital in Taiwan. \nShe works as Craniofacial Orthodontist in Department of Aesthetic, Plastic and Reconstructive Surgery, Faculty of Medicine, University of Gazi, Ankara Turkey since 2004.",institutionString:"Univeristy of Gazi",institution:null},{id:"255366",title:"Prof.",name:"Tosun",middleName:null,surname:"Tosun",slug:"tosun-tosun",fullName:"Tosun Tosun",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/255366/images/7347_n.jpg",biography:"Graduated at the Faculty of Dentistry, University of Istanbul, Turkey in 1989;\nVisitor Assistant at the University of Padua, Italy and Branemark Osseointegration Center of Treviso, Italy between 1993-94;\nPhD thesis on oral implantology in University of Istanbul and was awarded the academic title “Dr.med.dent.”, 1997;\nHe was awarded the academic title “Doç.Dr.” (Associated Professor) in 2003;\nProficiency in Botulinum Toxin Applications, Reading-UK in 2009;\nMastership, RWTH Certificate in Laser Therapy in Dentistry, AALZ-Aachen University, Germany 2009-11;\nMaster of Science (MSc) in Laser Dentistry, University of Genoa, Italy 2013-14.\n\nDr.Tosun worked as Research Assistant in the Department of Oral Implantology, Faculty of Dentistry, University of Istanbul between 1990-2002. \nHe worked part-time as Consultant surgeon in Harvard Medical International Hospitals and John Hopkins Medicine, Istanbul between years 2007-09.\u2028He was contract Professor in the Department of Surgical and Diagnostic Sciences (DI.S.C.), Medical School, University of Genova, Italy between years 2011-16. \nSince 2015 he is visiting Professor at Medical School, University of Plovdiv, Bulgaria. \nCurrently he is Associated Prof.Dr. at the Dental School, Oral Surgery Dept., Istanbul Aydin University and since 2003 he works in his own private clinic in Istanbul, Turkey.\u2028\nDr.Tosun is reviewer in journal ‘Laser in Medical Sciences’, reviewer in journal ‘Folia Medica\\', a Fellow of the International Team for Implantology, Clinical Lecturer of DGZI German Association of Oral Implantology, Expert Lecturer of Laser&Health Academy, Country Representative of World Federation for Laser Dentistry, member of European Federation of Periodontology, member of Academy of Laser Dentistry. Dr.Tosun presents papers in international and national congresses and has scientific publications in international and national journals. He speaks english, spanish, italian and french.",institutionString:null,institution:{name:"Istanbul Aydın University",country:{name:"Turkey"}}},{id:"171887",title:"Prof.",name:"Zühre",middleName:null,surname:"Akarslan",slug:"zuhre-akarslan",fullName:"Zühre Akarslan",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/171887/images/system/171887.jpg",biography:"Zühre Akarslan was born in 1977 in Cyprus. She graduated from Gazi University Faculty of Dentistry, Ankara, Turkey in 2000. \r\nLater she received her Ph.D. degree from the Oral Diagnosis and Radiology Department; which was recently renamed as Oral and Dentomaxillofacial Radiology, from the same university. \r\nShe is working as a full-time Associate Professor and is a lecturer and an academic researcher. \r\nHer expertise areas are dental caries, cancer, dental fear and anxiety, gag reflex in dentistry, oral medicine, and dentomaxillofacial radiology.",institutionString:"Gazi University",institution:{name:"Gazi University",country:{name:"Turkey"}}},{id:"256417",title:"Associate Prof.",name:"Sanaz",middleName:null,surname:"Sadry",slug:"sanaz-sadry",fullName:"Sanaz Sadry",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/256417/images/8106_n.jpg",biography:null,institutionString:null,institution:null},{id:"272237",title:"Dr.",name:"Pinar",middleName:"Kiymet",surname:"Karataban",slug:"pinar-karataban",fullName:"Pinar Karataban",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/272237/images/8911_n.png",biography:"Assist.Prof.Dr.Pınar Kıymet Karataban, DDS PhD \n\nDr.Pınar Kıymet Karataban was born in Istanbul in 1975. After her graduation from Marmara University Faculty of Dentistry in 1998 she started her PhD in Paediatric Dentistry focused on children with special needs; mainly children with Cerebral Palsy. She finished her pHD thesis entitled \\'Investigation of occlusion via cast analysis and evaluation of dental caries prevalance, periodontal status and muscle dysfunctions in children with cerebral palsy” in 2008. She got her Assist. Proffessor degree in Istanbul Aydın University Paediatric Dentistry Department in 2015-2018. ın 2019 she started her new career in Bahcesehir University, Istanbul as Head of Department of Pediatric Dentistry. In 2020 she was accepted to BAU International University, Batumi as Professor of Pediatric Dentistry. She’s a lecturer in the same university meanwhile working part-time in private practice in Ege Dental Studio (https://www.egedisklinigi.com/) a multidisciplinary dental clinic in Istanbul. Her main interests are paleodontology, ancient and contemporary dentistry, oral microbiology, cerebral palsy and special care dentistry. She has national and international publications, scientific reports and is a member of IAPO (International Association for Paleodontology), IADH (International Association of Disability and Oral Health) and EAPD (European Association of Pediatric Dentistry).",institutionString:null,institution:null},{id:"202198",title:"Dr.",name:"Buket",middleName:null,surname:"Aybar",slug:"buket-aybar",fullName:"Buket Aybar",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/202198/images/6955_n.jpg",biography:"Buket Aybar, DDS, PhD, was born in 1971. She graduated from Istanbul University, Faculty of Dentistry, in 1992 and completed her PhD degree on Oral and Maxillofacial Surgery in Istanbul University in 1997.\nDr. Aybar is currently a full-time professor in Istanbul University, Faculty of Dentistry Department of Oral and Maxillofacial Surgery. She has teaching responsibilities in graduate and postgraduate programs. Her clinical practice includes mainly dentoalveolar surgery.\nHer topics of interest are biomaterials science and cell culture studies. She has many articles in international and national scientific journals and chapters in books; she also has participated in several scientific projects supported by Istanbul University Research fund.",institutionString:null,institution:null},{id:"260116",title:"Dr.",name:"Mehmet",middleName:null,surname:"Yaltirik",slug:"mehmet-yaltirik",fullName:"Mehmet Yaltirik",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/260116/images/7413_n.jpg",biography:"Birth Date 25.09.1965\r\nBirth Place Adana- Turkey\r\nSex Male\r\nMarrial Status Bachelor\r\nDriving License Acquired\r\nMother Tongue Turkish\r\n\r\nAddress:\r\nWork:University of Istanbul,Faculty of Dentistry, Department of Oral Surgery and Oral Medicine 34093 Capa,Istanbul- TURKIYE",institutionString:null,institution:null},{id:"172009",title:"Dr.",name:"Fatma Deniz",middleName:null,surname:"Uzuner",slug:"fatma-deniz-uzuner",fullName:"Fatma Deniz Uzuner",position:null,profilePictureURL:"https://mts.intechopen.com/storage/users/172009/images/7122_n.jpg",biography:"Dr. Deniz Uzuner was born in 1969 in Kocaeli-TURKEY. After graduating from TED Ankara College in 1986, she attended the Hacettepe University, Faculty of Dentistry in Ankara. \nIn 1993 she attended the Gazi University, Faculty of Dentistry, Department of Orthodontics for her PhD education. After finishing the PhD education, she worked as orthodontist in Ankara Dental Hospital under the Turkish Government, Ministry of Health and in a special Orthodontic Clinic till 2011. Between 2011 and 2016, Dr. Deniz Uzuner worked as a specialist in the Department of Orthodontics, Faculty of Dentistry, Gazi University in Ankara/Turkey. In 2016, she was appointed associate professor. Dr. Deniz Uzuner has authored 23 Journal Papers, 3 Book Chapters and has had 39 oral/poster presentations. She is a member of the Turkish Orthodontic Society. 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