Classification of colloids according to the dispersed phase and dispersion medium.
\r\n\tTo further unravel critical mechanisms triggering metastasis and spontaneous regression of neuroblastoma, the key players and associated signalling pathways that dominate these mechanisms should be fully characterized. The genomic alterations, oncogenes and tumour suppressors, which affect cellular pathways, such as cell growth, proliferation, angiogenesis, metastasis, apoptosis and differentiation, play a major role in determining tumoural behaviour of neuroblastoma. This book will focus on key players and mechanisms of metastasis and spontaneous regression of neuroblastoma.
",isbn:null,printIsbn:null,pdfIsbn:null,doi:null,price:0,priceEur:0,priceUsd:0,slug:null,numberOfPages:0,isOpenForSubmission:!1,isSalesforceBook:!1,isNomenclature:!1,hash:"79a60ba88e02272c74e9c290e102cb99",bookSignature:"Dr. Nevim Aygun and Dr. Akira Nakagawara",publishedDate:null,coverURL:"https://cdn.intechopen.com/books/images_new/7697.jpg",keywords:"neuroblastoma, metastasis, spontaneous regression, mechanisms, epithelial to mesenchymal transition (EMT), migration, invasion, intravasation, extravasation, signalling pathways, MYCN amplification, 1p deletion, other deletions, other chromosomal abnormalities, chromothripsis, genomic alterations, oncogenes, tumour suppressors, proliferation, angiogenesis, apoptosis, DNA repair, differentiation, epigenetic control, immunity, telomerase",numberOfDownloads:null,numberOfWosCitations:0,numberOfCrossrefCitations:0,numberOfDimensionsCitations:0,numberOfTotalCitations:0,isAvailableForWebshopOrdering:!0,dateEndFirstStepPublish:"April 26th 2018",dateEndSecondStepPublish:"May 14th 2018",dateEndThirdStepPublish:"July 13th 2018",dateEndFourthStepPublish:"October 1st 2018",dateEndFifthStepPublish:"November 30th 2018",dateConfirmationOfParticipation:null,remainingDaysToSecondStep:"4 years",secondStepPassed:!0,areRegistrationsClosed:!0,currentStepOfPublishingProcess:5,editedByType:null,kuFlag:!1,biosketch:null,coeditorOneBiosketch:null,coeditorTwoBiosketch:null,coeditorThreeBiosketch:null,coeditorFourBiosketch:null,coeditorFiveBiosketch:null,editors:[{id:"195365",title:"Dr.",name:"Nevim",middleName:null,surname:"Aygun",slug:"nevim-aygun",fullName:"Nevim Aygun",profilePictureURL:"https://mts.intechopen.com/storage/users/195365/images/system/195365.jpeg",biography:"Nevim Aygun received her Medical Biology and Genetics Ph.D. in Health Sciences. She is interested in cancer, molecular biology, human genetics, cytogenetics, molecular cytogenetics, genomics, and bioinformatics. She has participated in many research projects on neuroblastoma, human gross gene deletions, non-B DNA-forming sequences, solid tumors, HCV, and leukemia, resulted in six articles, one book chapter, and numerous reports. She performed many molecular biological methods: PCR, real-time PCR, bacterial transformation, plasmid vector transfection, RNA interference, fluorescence in situ hybridization (FISH), cytogenetic, DNA sequencing, and cell culture. She also performed genomics and biostatistics analyses using some bioinformatics tools and SPSS program. She reviewed several manuscripts for some medical, genetics, and genomics journals. 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From chapter submission and review, to approval and revision, copyediting and design, until final publication, I work closely with authors and editors to ensure a simple and easy publishing process. I maintain constant and effective communication with authors, editors and reviewers, which allows for a level of personal support that enables contributors to fully commit and concentrate on the chapters they are writing, editing, or reviewing. I assist authors in the preparation of their full chapter submissions and track important deadlines and ensure they are met. I help to coordinate internal processes such as linguistic review, and monitor the technical aspects of the process. As an ASM I am also involved in the acquisition of editors. 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Although the overall incidence of childhood cancer has been slowly increasing since 1975, cancer in children and adolescents is still rare, the incidence of primary malignant liver tumors per year is 1-1.5 per million children in the United States [1, 2, 3, 4]. This yields a relative low rate for hepatic tumors (1.3% of all pediatric malignancies). Tumors of the liver may be either malignant or benign. Two thirds of liver tumors in children are malignant. Of these malignant tumors, hepatoblastoma (HB) and hepatocellular carcinoma (HCC) are the most common and account for 70 persent of all hepatic neoplasms. Unlike liver tumors in adults, in which the predominant histology is hepatocellular carcinoma, hepatoblastoma accounts for two thirds of liver tumors in children. Other liver malignancies in children include sarcomas, germ cell tumors, as well as rhabdoid tumors. Benign tumors of the liver in children include vascular tumors, hamartomas, adenomas, and focal nodular hyperplasia (FNH). The histology and anatomy of a pediatric liver tumor guides the treatment and prognosis [5, 6, 7, 8].
\n\t\t\tRecently, dramatic improvements in survival have been achieved for children and adolescents with liver cancer. Children and adolescents with liver cancer should be referred to multidisciplinary team incorporates the skills of the primary care physician, pediatric surgical subspecialists, radiation therapists, pediatric oncologists/hematologists, rehabilitation specialists, pediatric nurse specialists, social workers, and others to ensure that children receive treatment, supportive care, and rehabilitation that will achieve optimal survival and quality of life. Almost all liver masses in children are surgically treated, either primarily or following systemic chemotherapy [9, 10]. The conditions that eventuate in this choice of therapy, when and how to accomplish it, and the medical and surgical consequences for children of transplantation for tumors are described in guidelines for pediatric cancer centers and their role in the treatment of pediatric patients with cancer by the American Academy of Pediatrics [11, 12, 13]. Clinical trials for children and adolescents with cancer are generally designed to compare potentially better therapy with therapy that is currently accepted as standard. Clinical trials are available in many clinical institutes for liver cancer that occur in children and adolescents, and the opportunity to participate in these trials is offered to most patients/families [14].
\n\t\tBenign lesions in children represent 30% of hepatic tumors and are most commonly vascular in origin (eg, hemangiomas, hemangioendotheliomas). Two-thirds of hepatic neoplasms in children are malignant. Liver cancer is also rare malignancy in children and adolescents and account for approximately 1% of all pediatric malignancies. The malignant liver tumor is divided into two major histologic subgroups: hepatoblastoma, affecting around 80% of children, and hepatocellular carcinoma (HCC) [15, 16]. The age of onset of liver cancer in children is related to tumor histology. Hepatoblastoma usually occur before the age of 3 years, and approximately 90% of malignant liver tumors in children aged 4 years and younger are hepatoblastomas. There are 2 distinct groups of HCC patients in childhood: children who develop sporadic HCC without preceding liver disease, and those developing HCC in the context of advanced chronic liver disease (CLD). Sporadic HCC in children has a relatively poor outcome, while the several small series that report on HCC developing in CLD do so in the context of liver transplantation (LT). Some biologic differences may exist between HCCs developing in adults and children. One study reported an high radiological response (49%) in pediatric HCC, higher than adult HCC [17].
\n\t\t\tThe incidence of hepatocellular carcinoma is negligible in children aged 14 years and younger. In china, the incidence of hepatic tumors in children 14 years and younger is 2.6 per 100,000, of which 81 persent are hepatoblastoma. The incidence of hepatoblastoma in the United States increased in the last 25 years, whereas the incidence of hepatocellular carcinoma in the United States has not changed appreciably over time. The cause for the increase in incidence of hepatoblastoma is unknown, but the increasing survival of very low birth weight premature infants, which is known to be associated with hepatoblastoma, may contribute. In Japan, the risk of hepatoblastoma in children who weighed less than 1,000 g at birth are 15 times the risk in normal birth weight children. Other data has confirmed the high incidence of hepatoblastoma in very low birth weight premature infants. In several asian countries, the incidence of hepatocellular carcinoma in children is 10 times more than that in North America. The high incidence appears to be related to the incidence of perinatally acquired hepatitis B, which can be prevented in most cases by vaccination and administration of hepatitis B immune globulin to the newborn [18, 19].
\n\t\t\tAdditional rare malignant liver tumors in children are sarcoma, including its 3 variants rhabdomyosarcoma, embryonal or undifferentiated sarcoma, and angiosarcoma predominantly presenting in early childhood. Also included is the exceedingly uncommon cholangiocarcinoma, which can present at any age, often in the context of chronic biliary disease.The overall survival rate for children with hepatoblastoma is 70%, but is only 25% for those with hepatocellular carcinoma.
\n\t\tMost children with liver tumors commonly present insidiously with nonspecific abdominal discomfort, a palpable abdominal mass, feeding difficulties, and abdominal distension. Chronic fatigue secondary to anemia thrombocytopenia, and leukocytosis and lack of appetite are often reported. Jaundice and biochemical derangement are signs of advanced neoplastic change. Children with both HB and HCC may also present with weight loss, fever, and anorexia [20, 21, 22].
\n\t\t\tFetal and neonatal presentations include hydramnios, fetal hydrops, congestive heart failure, and respiratory distress. Occasionally, the child may present acutely with vomiting, fever and clinical signs of abdominal irritation, often suggestive of tumor rupture with intraperitoneal spread. Patients with congestive heart failure have been shown to have lower survival rates. Very rarely HB can present with signs of precocious puberty/virilization due to b-HCG secretion by the tumor. Laboratory studies are performed to assess baseline CBC count, electrolyte levels, liver enzyme levels, liver synthetic function, and α -fetoprotein (AFP) levels Serum AFP remains the key clinical marker of malignant neoplastic change, response to the treatment, and relapse. AFP levels are elevated in 50%-70% of children with hepatic neoplasms, and multiple studies confirm that AFP is a valuable surveillance marker in children who have previously undergone hepatic resection for malignancy. However, there are some variants of both HB and HCC that have low or normal AFP. These variants may have distinct histologic features and poorer prognoses [23, 24].\n\t\t\tThe initial workup for hepatic masses includes radiographic assessment using ultrasonography.
All children with a palpable abdominal mass usually undergo an initial ultrasound to confirm the location and to characterize the consistency as cystic or solid. Cystic or vascular lesions may not require any further imaging. However, definitive characterization of the mass requires a computed tomography (CT) or magnetic resonance imaging (MRI) scan. Calcifications can be seen in a minority of liver tumors. Hypervascularized hepatic lesions with delayed contrast excretion are highly suspicious of a malignant tumor.
\n\t\t\tAbdominal ultrasonography usually demonstrates a large mass, possibly with some satellite lesions and areas of hemorrhage within the tumor. CT scanning of the abdomen and chest are used for indeterminate or solid lesions to further delineate the location and to assess resectability (Fig. 1) and evaluate for the presence of pulmonary metastasis. MRI angiography is frequently helpful preoperatively to determine resectability because it delineates the vascular anatomy more precisely. Local radiological availability, expertise extent, and multiplicity of the lesions and to detect metastases may facilitate surgical planning and may determine resectability, however, definitive diagnosis can be proven only through biopsy findings [25, 26, 27]. \n\t\t\tCT scan of a hepatoblastoma amenable to surgical resection.
Any child with a suspected liver tumor should also have AFP and ß-HCG serum assays. The alpha-fetoprotein (AFP) and beta-hCG tumor markers are very helpful in diagnosis and management of liver tumors. Alttough elevation of AFP levels is not diagnostic of hepatic malignancy. AFP is markedly elevated in90% of hepatoblastoma cases and in many cases of hepatocellular carcinoma, and it returns to normal with effective therapy. The level of AFP at diagnosis and rate of decrease in AFP during treatment should be compared to the age-adjusted normal range. Caution should be taken in normal term infants who can have AFP levels in excess of 100,000 ng/ml, however, with a half-life of approximately 1 week, the AFP level normalizes to 10 ng/ml over the first few months of life. Absence of elevated AFP levels at diagnosis occurs in a few percentage of children with hepatoblastoma and appears to be associated with poor prognosis, as well as with the small cell undifferentiated variant of hepatoblastoma. Lack of a significant decrease of AFP levels with treatment may predict a poor response to therapy.
\n\t\t\tBeta-hCG is a hormone commonly produced by liver tumors and, in excess, can result in precocious puberty. It’s levels may also be elevated in children with hepatoblastoma or hepatocellular carcinoma, which may result in isosexual precocity in boys. Extremely high levels of beta-hCG are associated with infantile choriocarcinoma of the liver [28, 29].
\n\t\t\tBecause of the association between familial adenomatous polyposis and hepatoblastoma, obtaining a thorough family history is an important aspect of the management of a child with a liver tumor and his family, with particular attention to any family history of colon cancer or colonic polyps.
\n\t\t\tA chest CT is an important aspect of the workup because the lung parenchyma is the most common distant site for metastasis. A CBC typically displays mild normocytic and normochromic anemia with thrombocytosis.
\n\t\t\tTissue diagnosis of the tumor is essential, although some advocate that in the presence of very high AFP in a young child (6 months to 3 years). The practice in the United States is not to treat without a tissue sample except under the most urgent life-threatening circumstances, such as tumor growth into the right atrium. But this may not be necessary, as avoiding the biopsy theoretically reduces the risks of the tumor seeding. In Europe, The Childhood Liver Tumor Study Group of the Inter-national Society of Pediatric Oncology (SIOPEL) has developed a preoperative evaluation of the tumor extent (PRETEXT) grading system. The rationale for this recommendation is provided in the section on pathology. Segmental assessment of the extent of the tumor and its relation with the main hepatic vessels is of foremost importance for planning the intensity of chemotherapy and eventual surgery., which could provide a valuable tool for the risk stratification. Formal staging of the tumor should include chest and brain CT and bone scanning [30, 31].
\n\t\t\tBenign hepatic tumors are usually diagnosed incidentally. Some children may develop the Kasabach-Merritt phenomenon, a triad of coagulopathy, hemolytic anemia and thrombocytopenia due to intralesional pooling of the blood. IHE can have an acute presentation, typically within the first couple of weeks or months of life. Dramatic abdominal distension can lead to major respiratory distress, prompting the need for assisted ventilation and intensive care support. Nowadays some IHEs may be detected on routine antenatal ultrasonography, due to their characteristic vascular multichannel appearance. A proportion of children develop a bizarre secondary hypothyroidism that is thought to be secondary to tumor production of the enzyme iodothyronine deiodinase, which stimulates the conversion of thyroxine to reverse triiodothyronine and of triiodothyronine to 3,3’-diio-dothyronine, leading to a biochemical picture of hypothyroidism, requiring thyroxin supplementation. This phenomenon resolves once the tumor is removed or significantly decreases in size, usually within the first 2 years of life.
\n\t\t\tSimilar to other embryonal tumors, altered imprinting at the 11–15 locus has been observed in hepatoblastoma. Rearrangements involving the pericentric region of chromosome 1 also appear to be important in hepatoblastoma, with roughly 18% of hepatoblastomas displaying an imbalanced translocation involving this region. Hepatoblastoma is associated with several genetic syndromes and familial cancer predisposition conditions, such as familial adenomatous polyposis and Beckwith-Wiedemann syndrome in addition to several other rare syndromes. Other compelling evidence suggests that acquired aberrations in the ß-catenin/Wnt pathways are important in the pathogenesis of hepatoblastoma. Acquired chromosomal changes in tumors include numerical chromosomal changes, most commonly trisomies of chromosomes 2, 8, and 20. Finally, epigenetic changes in methylation patterns of DNA may be altered in hepatoblastoma.
\n\t\t\t\tThere is limited but compelling evidence that parental exposures are associated with a higher incidence of liver tumors and, more specifically, hepatoblastoma. Children from parents who have been exposed to metals used in soldering and welding, petroleum, or paints are at a higher risk for hepatoblastoma. Recent reports have also implicated parental smoking as a risk factor for hepatoblastoma [32, 33].
\n\t\t\tThe incidence of hepatoblastoma is increased 1,000 to 10,000-fold in infants and children with Beckwith-Wiedemann syndrome (BWS). BWS can be caused by either genetic mutations and be familial, or much more commonly, by epigenetic changes and be sporadic. Hepatoblastoma is also increased in hemihypertrophy, an overgrowth syndrome caused by the same epigenetic changes in chromosome 11p15.5 that cause many cases of BWS, but in a genetically mosaic fashion. Either mechanism can be associated with an increased incidence of embryonal tumors including Wilms tumor and hepatoblastoma. The gene dosage and ensuing increase in expression of insulin-like growth factor 2 (IGF 2) has been implicated in the macrosomia and embryonal tumors in BWS and hemihypertrophy. When sporadic, the types of embryonal tumors associated with BWS have frequently also undergone somatic changes in the BWS locus and IGF 2. All children with BWS or isolated hemihypertrophy should be screened regularly by ultrasound to detect abdominal malignancies at an early stage. Screening using AFP levels has helped in the early detection of hepatoblastoma in children with BWS or hemihypertrophy. Other somatic overgrowth syndromes, such as Simpson-Golabi-Behmel syndrome, may also be associated with hepatoblastoma.
\n\t\t\tThere is an association between hepatoblastoma and familial adenomatous polyposis (FAP); children in families that carry the APC gene are at an 800-fold increased risk for hepatoblastoma. However, hepatoblastoma occurs in less than 1% of FAP family members, so ultrasound and AFP screening for hepatoblastoma in members of families with FAP is controversial. The predisposition to hepatoblastoma may be limited to a specific subset of APC mutations. It has been recommended that all children with hepatoblastoma be examined for congenital hypertrophy of the retinal pigment epithelium, a marker of APC mutation carriers in 70% of polyposis families. In the absence of APC germline mutations, childhood hepatoblastomas do not have somatic mutations in the APC gene; however, they frequently have mutations in the beta-catenin gene, the function of which is closely related to APC.
\n\t\t\tHepatocellular carcinoma is associated with hepatitis B and hepatitis C infection, especially in children with perinatally acquired hepatitis B virus [33]. Compared with adults, the incubation period from hepatitis virus infection to the genesis of hepatocellular carcinoma is extremely short in a small subset of children with perinatally acquired virus. Widespread hepatitis B immunization has decreased the incidence of hepatocellular carcinoma in Asia. Mutations in the met/hepatocyte growth factor receptor gene occur in childhood hepatocellular carcinoma, and this could be the mechanism that results in a shortened incubation period.Hepatocellular carcinoma may also arise in very young children with mutations in the bile salt export pump ABCB11, which causes progressive familial hepatic cholestasis. Several specific types of nonviral liver injury and cirrhosis are associated with hepatocellular carcinoma in children including tyrosinemia and biliary cirrhosis.
\n\t\t\tUndifferentiated embryonal sarcoma of the liver (UESL) is the third most common liver malignancy in children and adolescents, comprising 9% to 13% of liver tumors. Widespread infiltration throughout the liver and pulmonary metastasis are common, usually between the ages of 5 and 10 years. It could also presents as an abdominal mass, often with pain or malaise. It may appear solid or cystic on imaging, frequently with central necrosis. Distinctive features are characteristic intracellular hyaline globules and marked anaplasia on a mesenchymal background. Many UESL contain diverse elements of mesenchymal cell maturation, such as smooth muscle and fat.
\n\t\t\t\tStrong clinical and histological evidence suggest that some UESLs arise from mesenchymal hamartomas of the liver (MHL), which are large benign multicystic masses that present in the first 2 years of life. Many MHLs have a characteristic translocation with a breakpoint at 19q13.4 and several UESLs have the same translocation. In a report of 11 cases of UESL, five arose in association with MHL, and transition zones between the histologies were noted. Some UESLs arising from MHLs may have complex karyotypes not involving 19q13.4.
\n\t\t\tChoriocarcinoma of the liver is a very rare tumor that appears to originate in the placenta and presents with a liver mass in the first few months of life. Infants are often unstable due to hemorrhage from the tumor. Clinical diagnosis may be made without biopsy based on extremely high serum beta-hCG levels and normal AFP levels for age.
\n\t\t\tEpithelioid hemangioendothelioma (EHE) is a rare vascular cancer that occurs in the liver and other organs.
\n\t\t\t\tGenerally, children with liver masses display normal growth and development unless they show the phenotypes associated with Beckwith-Wiedemann syndrome or the other genetic cancer predisposition syndromes associated with liver tumors.
\n\t\t\tHepatic neoplasms develop in a myriad of chronic liver disorders of childhood, often without or with minimal symptoms. Therefore, regular screening with abdominal ultrasound and serum AFP measurement should be in place for all children with CLD at least annually. Therefore, awareness of antecedent conditions that permit screening is essential. Detection of a liver tumor prior to dissemination and/or massive growth is the single most important management tool for all tumor types at all ages. Children with chronic hepatitis B should be also regularly checked, but because communities in which immunization has yet to be provided are typically impoverished and medically underserved, recommendations for screening have not yet been implemented. Some of the conditions with known increased propensity to develop malignancies such as tyrosinemia type 1 (even on nitizinone treatment) or bile salt export pump (BSEP) deficiency should be assessed every 6 months. However, there is no formal guideline for the frequency and manner of screening at this time [34, 35].
\n\t\t\tExtraordinary advances in neonatal care in the past 25 years have led to a wholly new population of children, the long-term survivors of birth as early as 22 to 23 weeks of gestation with a weight less than 1000 g. In addition to many other chronic problems, they have extraordinary susceptibility to HB. HB is dramatically more common in expremature babies but arranging effective screening programs could prove to be difficult because of their increasing numbers and fact that their long term care is typically provided outside hepatological clinics. Monitoring much smaller cohorts of children with Beckwith-Wiedemann Syndrome for HB is more feasible, and one study has suggested abdominal ultrasonography and serum AFP every 3 months until 4 years of age.
\n\t\t\tThere are several conditions for which screening of children for primary liver cancer is recommended by virtue of the attendant risk. Hepatitis B virus can cause HCC as early as age 4 following perinatal transmission from infected carrier mothers. Vaccination and perinatal administration of hepatitis B immunoglobulin have already reduced the incidence dramatically. A relative risk for such prematures versus term babies of 16- to 52-fold is recognized around the world. HB occurs at the same age as HB in term babies or later. Screening of infants with hemihypertrophy or hemiaplasia, as part of the Beckwith-Wiedemann over-growth syndrome, has been carried out for many years via ultrasound to detect intraabdominal malignancies. These include Wilms’ tumor and adreno cortical carcinoma, in addition to the less common HB, which has a relative risk of 2280. HB is not the only proliferative lesion of the Beckwith-Wiedemann syndrome liver, as hemangioendothelioma and mesenchymal hamartoma have also been observed, either con-currently or sequentially [37, 38].
\n\t\t\tIn familial adenomatous polyposis (FAP), the first manifestation of an autosomal dominant mutation in a family may be HB in a baby, with the colonic polyps detected only afterwards in a parent. The relative risk for children in such cohorts is 800-fold, but many examples are due to new germ-line mutations at 5q21,22 or only in the tumor.
\n\t\t\tA series from the Children’s Oncology Group focused primarily on known FAP families but raised the issue of de novo cases or the potential for infants of parents too young to be aware of the symptoms of FAP themselves.
\n\t\t\tThe largest report of sporadic cases looked at 50 patients and found 5 germline antigen-presenting cell (APC) mutations. This led the authors to recommend routine screening for APC mutations in all cases of sporadic HB, including both a screen for APC deletion or duplication and sequencing through the gene itself. In the only prospective screening study to date, 20 children with confirmed or suspected FAP were followed for 10 years by ultrasonography, and no tumors were detected. In FAP, other forms of hepatocellular neoplasia are also observed, including adenoma and HCC, as well as biliary adenomas.
\n\t\t\tThe timelines of the development of these various cancers in distinct tissues are not linked, and therefore, surveillance for these cancers needs to continue throughout the patient’s life [39]. Chronic cholestatic syndromes may be the substrate for liver cancers, with HB, cholangiocarcinoma, and in the Alagille syndrome of a paucity of intrahepatic bile ducts due to Jagged 1 or NOTCH mutations. Also, we have observed HB in three 2-year olds with congenital hepatic fibrosis and autosomal recessive polycystic disease. HB and HCC have been seen in the explants of infants with cirrhosis due to biliary atresia as early as 1 year. On the basis of the growth rate of HCC and with the aim of detecting tumors when they are 3 cm in diameter, the American Association for the Study of Liver Disease and the European Association for the Study of the Liver recommend screening ultrasound examinations at 6-month intervals, and some institutions shorten this interval to 3 months when the patient is on a transplant waiting list. These organizations have also published diagnostic criteria for liver nodules detected during the screening process.
\n\t\t\tHCC can be diagnosed noninvasively by computed tomography (CT) or magnetic resonance imaging (MRI) if a lesion 2cm in diameter within a cirrhotic liver demonstrates rapid contrast enhancement during the arterial phase and washout on the delayed venous phase. These guidelines were developed for cirrhotic adults, and there are no validated evidence-based guidelines for screening for tumors in children and adolescents with chronic liver disease.
\n\t\t\tAccording to adult data, ultrasound is insensitive for the diagnosis of HCC in the cirrhotic liver and should not be used for the detection of focal liver lesions in this setting. MRI is more sensitive than multidetector 3-phase CT for the diagnosis of regenerative and dysplastic nodules and is comparable to CT for the detection of HCC. There is a lower false-positive rate with MRI. Interval growth is probably the best indicator of malignancy, and there is a definite need for the establishment of protocols for follow-up imaging in centers that care for children with diffuse liver disease.
\n\t\t\tIn the case of hereditary tyrosinemia type 1 due to fumaryl acetoacetate hydrolase deficiency, prompt medical management, by blocking an enzyme upstream in the tyrosine catabolic pathway, can avert the injury that otherwise leads to HCC more often than any other metabolic defect. However, a low risk of developing HCC remains even with adequate medical management, so these children require life-long surveillance. Therefore, for the conditions listed, periodic abdominal ultrasonography and serum alpha fetoprotein measurements, at 3-month intervals in the case of Beck-with-Wiedemann syndrome and similarly for the first 3 years of life for others and then every 6 months thereafter, are advocated [40, 41]. In addition, recognition of the rare sequential occurrences of mesenchymal hamartoma and sarcoma and of hemangioendothelioma with angiosarcoma indicates the need for surveillance ultrasonography whenever a complete resection or transplant has not taken place [42, 43].
\n\t\tThe process used to find out if cancer has spread within the liver or to other parts of the body is called staging. The staging system would be useful in determining treatment plans and offers good prognostic value for overall and disease-free survival outcome. Historically, north Americans have staged liver tumors similar to other solid tumors, with surgical resectability and the presence of metastases as the primary criteria. The European staging system considers only the pretreatment extent of disease, and was developed by the Childhood Liver Tumor Strategy Group. After childhood liver cancer has been diagnosed, tests are done to find out if cancer cells have spread within the liver or to other parts of the body. The PRETEXT staging system divides the liver into four sectors, and the number of segments involved by tumor indicates stage. A lettering system further indicates extrahepatic involvement.The information gathered from the staging process determines the stage of the disease [44, 45].
\n\t\t\tThe following tests and procedures may be used in the staging process: -CT scan (CAT scan): This procedure is also called computed tomography, computerized tomography, or computerized axial tomography. The pictures are made by a computer linked to an x-ray machine. A procedure that makes a series of detailed pictures of areas inside the body, taken from different angles. A dye may be injected into a vein or swallowed to help the organs or tissues show up more clearly.
\n\t\t\t-MRI (magnetic resonance imaging): Also called nuclear magnetic resonance imaging (NMRI), a procedure that uses a magnet, radio waves, and a computer to make a series of detailed pictures of areas inside the body.
\n\t\t\t-Ultrasound exam: A procedure in which high-energy sound waves (ultrasound) are bounced off internal tissues or organs and make echoes. The echoes form a picture of body tissues called a sonogram. The picture can be printed to be looked at later.
\n\t\t\t-Surgery: An operation will be done to look at or remove the tumor. Tissues removed during surgery will be checked by a pathologist.
\n\t\t\tThere are 2 staging systems for childhood liver cancer.
\n\t\t\t-Presurgical (before surgery) staging: This staging system is called PRETEXT, based on imaging procedures such as MRI or CT, where the tumor has shown within the four parts (sections) of the liver.
\n\t\t\tThe liver is divided into 4 vertical sections.
\n\t\t\tIn PRETEXT stage 1(Fig. 2A), the cancer is found in one section of the liver. Three sections of the liver that are next to each other do not have cancer in them.
\n\t\t\t\n\t\t\tIn PRETEXT stage 2 (Fig. 2B), cancer is found in one or two sections of the liver. Two sections of the liver that are next to each other do not have cancer in them.
\n\t\t\t\n\t\t\tIn PRETEXT stage 3(Fig. 2C), the cancer is found in three sections of the liver and one section does not have cancer. OR, cancer is found in two sections of the liver and two sections that are not next to each other do not have cancer in them.
\n\t\t\tPostsurgical (after surgery) staging: The stage is based on the amount of tumor that remains after the patient has had surgery to look at or remove the tumor.
\n\t\t\tStage I
\n\t\t\tIn stage I, all of the cancer was removed by surgery in the liver.
\n\t\t\tStage II
\n\t\t\tIn stage II, a small amount of cancer remains in the liver, but it can be seen only with a microscope, or the tumor cells may have spilled into the abdomen before surgery or during surgery.
\n\t\t\tStage III
\n\t\t\tIn stage III:
\n\t\t\tIn stage III, the tumor cannot be removed by surgery; orcancer that can be seen without a microscope remains after surgery; or the cancer has spread to nearby lymph nodes.
\n\t\t\tStage IV
\n\t\t\tIn stage IV, the cancer has spread to other parts of the body. Cancer invades the surrounding normal tissue. Cancer invades the lymph system and travels through the lymph vessels to other places in the body. Cancer invades the veins and capillaries and travels through the blood to other places in the body.
\n\t\t\tThe metastasis is described as when cancer cells break away from the primary (original) tumor and travel through the lymph or blood to other places in the body, another (secondary) tumor may form [46]. The secondary (metastatic) tumor is the same type of cancer as the primary tumor. For example, if breast cancer spreads to the bones, the cancer cells in the bones are actually breast cancer cells. The disease is metastatic breast cancer, not bone cancer.
\n\t\tIn PRETEXT stage 4(Fig. 2D), cancer is found in all four sections of the liver.
\n\t\t\tThe key to successful treatment of malignant liver tumors in children is surgical removal, either by tumor resection/partial hepatectomy or Live Transplantation. Historically, complete surgical resection of the primary tumor has been required to cure malignant liver tumors in children. Complete surgical resection of the primary tumor continues to be the goal of definitive surgical procedures, but surgical resection is often combined with other treatment modalities (e.g., chemotherapy) to achieve this goal. SIOPEL recommends initial chemotherapy, while the American guidelines from COG require primary resection if possible, followed by chemotherapy, unless the tumor is pure fetal type HB stage 1, when the chemotherapy is not given. Both strategies have been successful in increasing the 5-year survival rates in HB to approximately 80% due to effective chemotherapy (cisplatinum in combination with doxorubicin or vincristine). Moreover, the timing and nature of surgical interventions are better defined for HB, and they are well-placed within the management protocols. For HCC, however, complete surgical excision or transplantation are essential for cure, and chemotherapy is not effective. On the whole, treatment planning by a multidisciplinary team of cancer specialists with experience treating tumors of childhood is required to determine and implement optimum treatment [47, 48].
\n\t\t\tThe most important step in the management of benign tumors in children is confirmation of their genuine benign nature. Multiphase contrast CT imaging and, less frequently, direct angiography are required for the radiological diagnosis. Some of the benign tumors, including IHE, mesenchymal hamartoma, and FNH, would have characteristic radiological features, not always requiring a tissue diagnosis.
\n\t\t\tMany of the improvements in survival in childhood cancer have been made using new therapies that have attempted to improve on the best available, accepted therapy. Clinical trials in pediatrics are designed to compare potentially better therapy with therapy that is currently accepted as standard.Because of the relative rarity of cancer in children, all children with liver cancer should be considered for entry into a clinical trial. This comparison may be done in a randomized study of two treatment arms or by evaluating a single new treatment, comparing the results with those previously obtained with standard therapy [49].
\n\t\t\tThe timing of the surgical approach is critical. For this reason, surgeons with experience in pediatric liver resection and transplantation should be involved early in the decision-making process for determining optimal timing and extent of resection.There are three ways in which surgery is used to treat primary pediatric liver cancer, including initial surgical resection (alone or followed by chemotherapy), delayed surgical resection (chemotherapy followed by surgery) and orthotopic liver transplantation [50].
\n\t\t\t\tThe lesion to resect is marked out.
Electrocautery is useful for dissecting through the liver capsule and parenchyma.
Resection is typically performed through a bilateral subcostal incision, and, occasionally, a right thoracoabdominal approach is necessary for large lesions arising high in the right lobe. Surgical resection has seen applications of newer technology. Intraoperative ultrasonography has been widely applied to determine the exact location of the tumor relative to the vessels. Once deemed resectable, the resection is marked out (Fig. 3, 4), and various tools may then be used to perform the resection; electrocautery, bipolar devices such as LigaSure, and argon beam coagulation for hemostasis have been used.
\n\t\t\t\t\n\t\t\t\tThe most frequently performed procedure is a right hepatectomy (60%) because hepatoblastomas (HBs) occur 3 times more often in the right lobe than in the left. The hilar plate is divided, exposing the bifurcation of the hepatic artery and portal vein. These structures are ligated (Fig. 5).
\n\t\t\t\tSuture and ligation may be useful in sealing blood vessels and hepatic ducts.
In an extended right hepatectomy, the middle hepatic vein is ligated and segment 4 is resected. The right hepatic vein is identified and ligated before any division of the hepatic parenchyma. At completion, only segments 2 and 3 and the caudate lobe remain.
\n\t\t\t\tLeft hepatic lobectomy begins the same way right hepatectomy, with division of the left hepatic artery and left branch of the portal vein. The left and middle hepatic veins are identified after dissection through the sinus venosus. The liver is then transected after vascular isolation of the resected segments. An extended left hepatectomy includes removal of all or most of segments 5 and 8. Unresectability is usually determined by involvement of hilar structures or all hepatic veins, multicentricity, and invasion of inferior vena cava (IVC) or portal vein. Centrally located tumors are, by definition, more likely unresectable.
\n\t\t\t\tLaparoscopic and robotic resections of both benign and malignant liver tumors have been described. Their role in standard practice is still being defined.
\n\t\t\t\tIf preoperative chemotherapy is to be administered, it is very important to consult frequently with the surgical team concerning the timing of resection, as prolonged chemotherapy can lead to unnecessary delays and in rare cases, tumor progression. If the tumor can be completely excised by an experienced surgical team, less postoperative chemotherapy may be needed.
\n\t\t\t\tIn PRETEXT stage 3 or 4 disease patients with involvement of major liver vessels, early involvement with an experienced pediatric liver surgeon is especially important, patients with. Although initially thought to be a contraindication to resection, experienced liver surgeons could also perform aggressive approaches avoiding transplantation for vascular involvement patients. Accomplishing a complete resection is imperative since rescue transplant of incompletely resected patients has an inferior outcome compared to patients who are transplanted as the primary surgical therapy.
\n\t\t\t\tSurgical resection of distant disease has also contributed to the cure of children with hepatoblastoma and is often performed at the same time as resection of the primary tumor. Resection of pulmonary metastases is recommended when the number of metastases is limited. When possible, resection of areas of locally invasive disease, such as in the diaphragm, and of isolated brain metastasis is recommended. Second resection of positive margins and/or radiation therapy may not be necessary in patients with incompletely resected hepatoblastoma whose residual tumor is microscopic and who receive subsequent chemotherapy.
\n\t\t\t\tMajor intraoperative complications include hemorrhage, air embolism, tumor embolus, and bile duct injury. Only 20% of the liver is necessary to maintain hepatic function; thus, postoperative insufficiency is rare. Postoperative complications include hemorrhage, bile leak, abscess formation, pulmonary complications, and wound problems. Postoperative care consists of adequate fluid replacement, intravenous albumin supplementation, vitamin K, and clotting factors for the first 3-4 days. The liver function test results generally normalize within the first 2 weeks, and hepatic insufficiency is reasonably rare. Postoperative monitoring consists of frequent ultrasonography, chest radiography, and serial α -fetoprotein (AFP) level measurements, generally at 3-month to 6-month intervals.
\n\t\t\t\tTumor rupture at presentation, resulting in major hemorrhage that can be controlled by transcatheter arterial embolization or partial resection to stabilize the patient, does not preclude a favorable outcome when followed by chemotherapy and definitive surgery. The decision as to which surgical approach to use depends on many factors including: PRETEXT stage, size of the primary tumor, presence of multifocal hepatic disease, AFP levels, Vascular involvement, preoperative chemotherapy as well as orthotopic liver transplantation criteria.
\n\t\t\t\tIn North American clinical trials, the Children\'s Oncology Group (COG) has recommended that surgery be performed initially if a complete resection can be accomplished. COG is investigating the use of PRETEXT stage at diagnosis and after chemotherapy to determine the optimal surgical approach and its timing. In European clinical trials, only patients with PRETEXT stage 1 receive resection surgery and all other patients are biopsied [51, 52, 53].
\n\t\t\t\tIt is difficult to compare the North American and European approaches. Somewhat comparable results for children with PRETEXT stage 1 and 2 tumors were obtained in two international studies. The 5-year survival of PRETEXT stage 1 and 2 patients(chemotherapy prior to attempted surgical resection of the primary liver tumor) is 90% to 100% on the European studies and seems to be similar to that of children treated on North American studies where surgery was performed before chemotherapy. In comparison, a survey of children with liver tumors who were treated prior to the consistent use of combination chemotherapy found that 45 of 78 patients (57%) with hepatoblastoma who had complete excision of the tumor survived while no children with positive margins or gross disease following resection survived.
\n\t\t\tOrthotopic liver transplantation was first described in 1968 by Starzl. Liver transplantation has recently been associated with significant success in the treatment of children with unresectable hepatic tumors. The criteria currently used to evaluate adult transplant candidates may not be applicable for pediatric patients. The main indication for transplantation is nonmetastatic, unresectable lesions. Extrahepatic disease and lymph node involvement did not prove to be contraindications. Hepatoblastoma (HB) now constitutes an indication for 3% of all pediatric liver transplantations, whereas the role of liver transplantation for HCC is more controversial. In hepatocellular carcinoma, vascular invasion, distant metastases, lymph node involvement, tumor size, and male gender were significant risk factors for recurrence. Because of the poor prognosis in patients with hepatocellular carcinoma, liver transplant should be considered for disorders such as tyrosinemia and familial intrahepatic cholestasis early in the course, prior to the development of liver failure and malignancy. Because no good medical therapy for pediatric HCC has been identified, liver transplantation should be carefully evaluated as front-line therapy. Additionally, successful transplantation has been used benign lesions such as diffuse hepatic hemangiomas. In addition, liver transplantation may be an option in children with unresectable primary tumors, without metastatic disease, after neoadjuvant chemotherapy and pulmonary metastasectomy, if necessary. It has been suggested that adjuvant chemotherapy following transplant may decrease the risk of tumor recurrence. Generally, preoperative and postoperative chemotherapy are recommended, in addition to postoperative immunosuppression [54, 55, 56].
\n\t\t\t\tTransplantation may also be used in selected cases of tumor recurrence but is much less successful when used for salvage therapy. There are discrepant results on the outcomes for patients with lung metastases at diagnosis who undergo orthotopic liver transplantation following complete resolution of lung disease in response to pretransplant chemotherapy. Some studies have reported favorable outcomes for this group of patients, while others have noted high rates of hepatoblastoma recurrence. All of these studies are limited by small patient numbers; further study is needed to better define outcomes for this subset of patients [57, 58].
\n\t\t\t\tA review of the world experience has documented a posttransplant survival rate of 70% to 80% for children with hepatoblastomas. Intravenous invasion, positive lymph nodes, and contiguous spread did not have a significant adverse effect on outcome.
\n\t\t\t\tThe primary cause of death for both HB and HCC was metastatic disease. Generally, the 5-year survival rate for patients transplanted for HB is 70%.
\n\t\t\t\tA study of the United Network for Organ Sharing (UNOS) database reported 135 patients undergoing 135 transplants for HB and 43 transplants for HCC with 1-year, 5-year, and 10-year survival of 79%, 69%, and 66% for HB, respectively, and 86%, 63%, and 58% for HCC, respectively [59, 60]. Liver transplantation for hepatic hemangioma has been studied in 59 patients in Europe with 1-year, 5-year, and 10-year patient survival rates of 93%, 83%, and 72%, respectively.
\n\t\t\t\tThe availability of donor organs has increased with the use of split-liver grafting and other "technical variant" techniques, along with living-related liver transplant techniques. Prognosis in terms of graft and patient survival appear to be the same between full-size liver and technical variant liver transplants; however, morbidity following transplant appears to be higher in those patients who receive technical variant grafts [61, 62, 63, 64].
\n\t\t\t\tEarly failure of liver transplant (< 30 d) is usually due to vascular complications or primary nonfunction. Late failure is usually more a result of infection, posttransplant lymphoproliferative disease, chronic rejection, biliary complications, or recurrence of malignant disease. These failures may warrant retransplantation. The predictors of success after retransplantation remain unknown. The United Network for Organ Sharing (UNOS) Standard Transplant and Research Files registry reported all children younger than 18 years listed for a liver transplant in the United that the 5-year survival rates of 69% for hepatoblastoma and 63% for hepatocellular carcinoma and the 10-year survival rates were similar to the 5-year rates. Application of the Milan criteria for UNOS selection of recipients of deceased donor livers is controversial. However, living donor liver transplants are more common with children and the outcome is similar [65, 66, 67, 68, 69].
\n\t\t\tIn recent years, virtually all children with hepatoblastoma have been treated with chemotherapy, which may reduce the incidence of surgical complications at the time of resection, and in some centers, even children with resectable hepatoblastoma are treated with preoperative chemotherapy. For PRETEXT stage 1 hepatoblastoma, it was resected and treated with doxorubicin and cisplatin chemotherapy. The pre-resection neoadjuvant chemotherapy (doxorubicin and cisplatin) was given to all children with PRETEXT stage 2, 3, or 4 hepatoblastoma with or without metastases. The chemotherapy was well tolerated. This strategy resulted in an OS of 75% at 5 years after diagnosis. Identical overall results were seen in a follow-up international study. Following chemotherapy, and excluding those who received liver transplant (less than 5% of patients), complete resection was obtained in 87% of children. In contrast, an American Intergroup protocol for treatment of children with hepatoblastoma, encouraged resection at the time of diagnosis for all tumors amenable to resection without undue risk. The protocol did not treat children with stage I tumors of purely fetal histology with preoperative or postoperative chemotherapy unless they developed progressive disease. Further study will be needed to determine whether presurgical chemotherapy is preferable to resection followed by chemotherapy for children with PRETEXT stage 2, 3, and 4 hepatoblastoma [70, 71].
\n\t\t\t\tRoutine assessment of hearing, renal, and cardiac function is standard during treatment for pediatric malignancies. Post-chemotherapy neutropenia rarely represents additional concerns during the surgical treatment. Platinum compounds (cisplatin and carboplatin), which have been a backbone of the successful treatment for pediatric liver tumors, are also quite ototoxic. Around 40% of children develop significant hearing loss, which typically affects high-register tones, and could be delayed. Chronic dose-related nephrotoxicity remains a significant long-term issue for both chemotherapy for malignant liver tumors and calcineurin inhibitor-based immunosuppression. Therefore, early use of calcineurin inhibitor-sparing agents, such as mycophenolate mofetil or sirolimus, is recommended for children after LT for liver tumors. Nevertheless, it is prudent not to give chemotherapy 2 weeks before or after resection or LT.
\n\t\t\t\tIn rare cases, intensive platinum- and doxorubicin-based multidrug chemotherapy can induce complete regressions in approximately 50% of patients, with subsequent 3-year event-free survival of 56% for pulmonary metastases and eliminated multinodular tumor foci in the liver. Chemotherapy has been much more successful in the treatment of hepatoblastoma than in hepatocellular carcinoma.
\n\t\t\tOther treatment approaches such as transarterial chemoembolization, have been used for patients with postsurgically-staged stage III hepatoblastoma. Transarterial chemoembolization has been used in a few children to successfully shrink tumor size to permit resection.Cryosurgery, intratumoral injection of alcohol, and radiofrequency ablation can successfully treat small (<5 cm) tumors in adults with cirrhotic livers. Some local approaches such as cryosurgery, radiofrequency ablation, and transarterial chemoembolization that suppress hepatocellular carcinoma tumor progression are used as bridging therapy in adults to delay tumor growth while on a waiting list for cadaveric liver transplant [72].
\n\t\t\tIt is no surprise that most of the toxicity data stem from HB treatment survivors, while information from the HCC setting is lacking.
\n\t\t\tThe prognosis for a patient with recurrent or progressive hepatoblastoma depends on many factors, including the site of recurrence, prior treatment, and individual patient considerations. If possible, isolated metastases should be resected completely in patients whose primary tumor is controlled. For example, in patients with stage I hepatoblastoma at initial diagnosis, aggressive surgical treatment of isolated pulmonary metastases that develop in the course of the disease may make extended disease-free survival possible. Liver transplant should be considered for patients with isolated recurrence in the liver. Combined vincristine/irinotecan has been used with some success. Some patients treated with cisplatin/vincristine/fluorouracil could be salvaged with doxorubicin-containing regimens, but patients treated with doxorubicin/cisplatin could not be salvaged with vincristine/fluorouracil. Treatment in a clinical trial should be considered if all of the recurrent disease cannot be surgically removed. Phase I and phase II clinical trials may be appropriate and should be considered [73, 74].
\n\t\t\t\tThe prognosis for a patient with recurrent or progressive hepatocellular carcinoma is poor. Chemoembolization or liver transplant should be considered for those with isolated recurrence in the liver. Phase I and phase II clinical trials may be appropriate and should be considered [75, 76].
\n\t\t\tManagement of pediatric liver tumors has significantly improved over the last 2 decades. The principal reasons are that efficient chemotherapy and established medico-surgical treatment algorithms for HB have now integrated LT as a very valuable complementary treatment option. The management options for HCC are less effective and not well defined, broadly mirroring the therapeutic guidelines in adults except for a more cautionary approach to neoadjuvant and loco-regional methods. In the pediatric context the main clinical aims are to reduce chemotherapy toxicity (predominantly ototoxicity and nephrotoxicity) in children treated for HB and to investigate additional modes of treatment for HCC.
\n\t\t\tImproved understanding of HB and HCC biology may improve risk stratification a presentation and direct the treatment at specific molecular targets in the future. Management of less common benign and malignant tumors should benefit from establishing international collaborative pediatric networks such as the Pediatric Liver Unresectable Tumor Observatory (PLUTO).
\n\t\tColloids are heterogeneous mixtures of at least two distinct phases, with the material of one of the phases in a finely divided form (solid, liquid or gas), called dispersed phase, mixed with the continuous phase (solid, liquid or gas), called medium dispersion [1].
Understanding and controlling the stability of colloidal dispersions is essential for its satisfactory use. For both economic and environmental reasons, water is often required as a dispersing phase, even when the particles that need to be kept in suspension are hydrophobic, as is the case with cellulose [1].
Cellulose has been gaining importance in the industrial scenario due to the growing interest in sustainability and environmental protection, becoming a competitive material since it is renewable, abundant, low cost, non-petroleum and non-toxic [2].
Suspended cellulose has a tendency to aggregate. In this way, some strategies to avoid cellulose self-agglomeration in aqueous medium have been used in order to reduce the hydrophilic character of cellulose, avoiding the formation of additional hydrogen bonds between cellulose fibers [3].
Therefore, this chapter aims to contribute to the field of study of colloids and their characteristics, in addition to cellulose with regard to its characteristics and behavior of aqueous solutions of cellulose and alternatives sought to improve the colloidal stability of cellulose suspensions.
Colloids are systems formed by macromolecules or particles dispersed in a medium, in which one or more components have at least one of their dimensions within the range of 1 nm to 1000 nm [4].
Colloidal systems have been used since the dawn of humanity. Ancient people used gels from natural products as food, clay dispersions for the manufacture of ceramic utensils and colloidal pigment dispersions to decorate cave walls [5].
Colloidal systems are present in our daily lives in several products and technologies, such as personal hygiene (shampoo, toothpaste, foam, shaving cream, makeup, cosmetics) and in food (milk, coffee, butter, vegetable creams, fruit jellies, beer, soda or ice cream). During a single day we are consuming several colloids [5]. Colloids are also present in several consumer goods production processes, including drinking water, in the separation processes in the biotechnology industries and in the treatment of the environment.
In addition, colloidal phenomena are frequently used in industrial processes for the production of polymers, detergents, paper, soil analysis, food products, fabrics, precipitation, chromatography, ion exchange, flotation and heterogeneous catalysis. In orthomolecular therapeutic medicine, knowledge of the properties of colloidal systems can assist in the elucidation of diseases, such as Alzheimer’s and Parkinson’s [5].
The factors that most contribute to the characteristics of a colloid are:
The particle dimensions;
The shape and flexibility of the particles;
Surface properties;
Particle-particle interactions;
Particle-solvent interactions.
Colloids have specific characteristics such as high mass, high particle area/volume ratio and are relatively large. On the separation surfaces (interfaces) between the dispersed phase and the dispersion medium, characteristic surface phenomena are manifested, such as adsorption and double electrical layer effects, phenomena of great importance in determining the physicochemical properties of the system as a whole [6].
Depending on the affinity between the particles of a dispersion and the medium in which they are dispersed, we can classify colloids in two ways: lyophilic and lyophobic colloids. Lyophilic colloids are those in which the particle surface has an affinity for the solvent, keeping the dispersion more stable and minimizing aggregation. Lyophobic colloids, on the other hand, are those in which the particles have greater interaction with each other, which ends up leading to a rapid aggregation process [7].
Regarding the colloid classification, there are the following categories:
Aerosol: consists of a solid or a liquid dissolved in a gas.
Foam: consists of a gas dispersed in solid or liquid.
Emulsion: are colloids formed by liquid dispersed in another liquid.
Sol: are colloids formed by the dispersion of a solid in a liquid or solid.
Gel: solid of gelatinous material formed from a colloidal dispersion, in which the dispersed is in the liquid state and the dispersant in the solid state.
The Table 1 shows some different types of colloids according to the state of the continuous and dispersed phases, and examples found in everyday life.
Scattered | ||||
---|---|---|---|---|
Gas | Liquid | Solid | ||
Dispersant | Gas | Does not exist. All gases are soluble with each other | Aerosol Liquid Examples: cloud, fog | Aerosol solid Examples: smoke, dust in suspension |
Liquid | Liquid foam Example: soap foam, shaving cream, whipped cream | Emulsion Examples: milk, honey, mayonnaise, creams | Sol Example: paints, colored glass | |
Solid | Solid foam Example: pumice, expanded polystyrene | Gel Examples: gelatin, cheese, jam | Solid Sun Example: ruby and sapphire crystal, metal alloys |
Classification of colloids according to the dispersed phase and dispersion medium.
Colloidal systems can be divided into three types: colloidal dispersions, true macromolecule solutions and association colloids [8].
Colloidal dispersions are heterogeneous systems composed of two or more phases, as shown in Table 1, and these systems are thermodynamically unstable, due to their high surface free energy. In a colloidal dispersion, the interfacial area of the dispersed phase is very large, which requires a lot of energy to keep it dispersed. In an attempt to minimize the free energy of the surface, the system tends to minimize the area, based on the aggregation of the dispersed phase [8].
True macromolecule solutions are thermodynamically stable colloidal systems, that is, they will not separate phase. Polymeric solutions are examples of this class of colloids. Association colloids, which are also thermodynamically stable, are formed by the association of surfactant molecules, that is, micellar aggregates [8].
For the production of colloids there are two groups with different production methods, they are: dispersion methods and condensation methods [3].
The condensation method is a means of producing colloids carried out with the precipitation of an insoluble substance by means of a chemical transformation between solvent substances. During its chemical transformation, the insoluble product is in the molecular state, occurring after condensation.
The different interactions between the dispersed phase (particles) and the dispersion phase (continuous) constitute one of the critical points in the study of the behavior and stability of colloids. The interactions between the particles that make up a dispersion and the dispersing medium are fundamental to understand colloidal stability [9].
The stability of a dispersion can be thermodynamic or kinetic and one of the ways to understand the difference between them is in terms of the colloid stabilization time. While a thermodynamically stable colloid will remain unchanged for an infinite time, maintaining properties like temperature and concentration unchanged, kinetically stable colloids tend to aggregate over time. Therefore, the study of colloidal chemistry makes it possible to change the time in which the colloid remains kinetically stable [8].
When it comes to particles, the energy in van der Waals’ interactions comes from integrating the potential of all the molecules that make it up [10]. Van der Waals interactions between two particles will always be attractive if the particles are made of the same material, no matter what medium they are in [11]. If the particles are different in nature, van der Waals interactions can be attractive or repulsive [12]. In the study of colloidal dispersions, the focus is mostly on the interaction of particles of the same nature, that is, they are attractive interactions [13].
To increase the stability of a colloidal dispersion the steric effect of macromolecules is used to prevent the particles from aggregating by adding a stabilizer that will adsorb on the surface of the particle [13]. If the adsorbed macromolecule is in a good solvent, its chains expand. When it encounters a chain from another particle, there is a restriction in the conformation of both chains in the volume between the two particles, causing a decrease in configurational entropy and an increase in free energy [14]. To minimize this effect, the chains of the macromolecules repel each other, causing a repulsive effect between the particles, preventing aggregation.
Regarding the stability of aqueous colloidal dispersions, they are sensitive to the presence of electrolytes and polyelectrolytes (charged polymers of high molecular mass), since the colloidal particles can irreversibly aggregate in the presence of electrolytes and result in large and compact aggregates (clots) by a process called coagulation, while in the presence of polyelectrolytes there may be the formation of less dense aggregates (floccules), which can be easily broken and dispersed by mechanical agitation [15].
Understanding and controlling the stability of colloidal dispersions is essential for its satisfactory use. Some specific applications require that such dispersions be maintained over a wide range of temperatures and chemical conditions [8].
For both economic and environmental reasons, water is often required as a dispersing phase, even when the particles that need to be kept in suspension are hydrophobic. Water is a highly structured material, due to the hydrogen bonds that connect the molecules to each other. In the vicinity of a hydrophobic surface, ruptures of the hydrogen bonds between water molecules occur, increasing the free energy in relation to the solution. As a consequence, water is expelled to regions more favorable to hydrogen bonding. The migration of water molecules results in a mutual attraction between hydrophobic surfaces that implies a reduction in the free energy of the system [11].
Cellulose has stood out in the last 20 years as a study material for several applications, as it is the most abundant, renewable and natural polymer on the face of the Earth [15], and can be found mainly in woody plants (wood), annuals and in grasses [16]. Cellulose is located mainly in the secondary cell wall, corresponding to approximately 40 to 45% of the wood mass [17].
Cellulose (C6H10O5) n is a polysaccharide, linear chain containing from hundreds to thousands of chemical bonds involving carbon, hydrogen and oxygen atoms (Figure 1) [18]. The cellulose chain is of high molecular weight, which tends to form hydrogen bonds between the molecules [19, 20]. The hydroxyl groups of cellulose molecules form hydrogen bonds that can be intramolecular or intermolecular, directing the crystalline packaging, and it is these bonds that make cellulose a stable polymer and appreciated as reinforcement in composites [21, 22].
Chemical structure of cellulose.
Its organized structure is formed by cellulose microfibrils, which due to intermolecular bonds form the fibrils, which in turn are composed in an orderly fashion in order to form cellulosic fibers. Cellulose fibers are made up of two regions, the crystalline region, in which the microfibrils are presented in an extremely orderly manner, and the amorphous region, in which they are arranged in a less ordered manner [17], and for some lignocellulosic sources the amorphous regions can reach 50% of the structure [22].
Despite the hygroscopic nature of the individual cellulose molecules, the absorption of water molecules is only possible in the amorphous zones, since there is a lack of empty spaces in the crystalline structure. Hydroxy groups are the most abundant groups in the cellulose molecule, followed by the acetal bonds that form the ring of pyraneses [23].
In the crystalline regions of cellulose, we also have that the intra and intermolecular interactions can vary, giving rise to the various polymorphs [18]. The degree of polymerization and the crystallinity of cellulose vary according to the lignocellulosic source [1]. Due to the presence of crystalline and amorphous regions, cellulose can be classified as a semicrystalline fibrillar material [24].
Using cellulosic materials has several advantages, such as: its low cost, low density, high mechanical resistance and high elastic modulus. Due to the stable structure of their crystalline regions, cellulose fibrils have high mechanical properties along the longitudinal direction [24]. It is also possible to benefit from the high stiffness of the cellulose crystal which, when used on a nanometer scale for the production of composite materials, makes it possible to preserve the optical properties of the original material while improving the mechanical properties [25].
Cellulosic pulp is a material whose characteristics and properties are determined by its origin. Cellulose modification methods are used when carrying out processes carried out in an aqueous medium, but cellulose is an amphiphilic polymer, that is, it presents a hydrophilic region that dissolves in water, and another hydrophobic region that does not dissolve in water, due to the presence of crystalline and amorphous regions.
The geometry, size and surface density of the particles are also properties that interfere with the processes of coagulation and flocculation. The polymers used with water retention agents increase the forces of colloidal attraction and induce flocculation through different mechanisms, based on different effects. We can mention: flocculation by bridge effect, flocculation by depletion effect and flocculation by reinforced bridge effect [1].
In the case of cellulose fibers, these properties are not well defined due to the variety in the size and shape of the fibers. However, it is known that cellulose fibers when dispersed in water have a pH of around 6, which indicates the acidic character of the surface, therefore a tendency to preferentially adsorb OH- group. In this way, the aqueous dispersions of cellulose fibers are influenced in their colloidal stability by the presence of a double electrical layer under their surface, resulting from the dissociation of different functional groups, such as carboxylics [26].
The pure cellulose fiber in suspension has a high tendency to aggregate and form clots by the action of gravity. However, studies show that through the addition of symmetrical or asymmetric electrolytes the tendency to coagulate the cellulose fiber suspension can be maximized or minimized depending on the final objective. The addition of cationic starch and calcium carbonate to the cellulose fiber suspension causes a change in the charge signal of the fiber surface, resulting in phenomena of fiber-fiber interaction that guarantees greater stability in relation to pure cellulose fiber [1].
In the refining process, for example for the production of paper, cellulose fibers are immersed in water. The fibrils, which make up the cells, are composed of crystalline regions that, when immersed in water, absorb a quantity of this water across all exposed crystalline surfaces, causing their swelling and decreased attraction between the fibrils. The mechanical action of shearing the fibers through refiners speeds up this swelling, as it exposes the surfaces previously located inside the fibers, causing an increase in surface exposure, which promotes a greater number of contacts and connections between the fibers, resulting in this stronger paper [1].
The steps of converting cellulose to paper involve many surface chemical interactions, interactions between fibers and colloidal particles. Understanding these interactions is useful for product development and improving the resolution of operational problems.
This chapter sought to define the main characteristics of colloids, as well as their classification, methods of preparation and finally to address characteristics of colloid stability. Cellulose, the most abundant biopolymer in the world, is a colloid widely used in several industries. This colloid proves challenging for some segments due to its detailed characteristics throughout of the chapter. Studies continue to be carried out on this topic in order to bring solutions to improve the colloidal stability of cellulose.
I thank IntechOpen for the opportunity and the Federal University of Paraná for my training from undergraduate to doctorate.
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In most of the developed countries, the age of 60 is considered equivalent to retirement age and it is said to be the beginning of old age. In this chapter, you understand the details of ageing processes and associated physiological changes.",book:{id:"6381",slug:"gerontology",title:"Gerontology",fullTitle:"Gerontology"},signatures:"Shilpa Amarya, Kalyani Singh and Manisha Sabharwal",authors:[{id:"226573",title:"Ph.D.",name:"Shilpa",middleName:null,surname:"Amarya",slug:"shilpa-amarya",fullName:"Shilpa Amarya"},{id:"226593",title:"Dr.",name:"Kalyani",middleName:null,surname:"Singh",slug:"kalyani-singh",fullName:"Kalyani Singh"},{id:"243264",title:"Dr.",name:"Manisha",middleName:null,surname:"Sabharwal",slug:"manisha-sabharwal",fullName:"Manisha Sabharwal"}]},{id:"55388",doi:"10.5772/intechopen.68944",title:"Beauty, Body Image, and the Media",slug:"beauty-body-image-and-the-media",totalDownloads:7768,totalCrossrefCites:5,totalDimensionsCites:12,abstract:"This chapter analyses the role of the mass media in people’s perceptions of beauty. We summarize the research literature on the mass media, both traditional media and online social media, and how they appear to interact with psychological factors to impact appearance concerns and body image disturbances. There is a strong support for the idea that traditional forms of media (e.g. magazines and music videos) affect perceptions of beauty and appearance concerns by leading women to internalize a very slender body type as ideal or beautiful. Rather than simply being passive recipients of unrealistic beauty ideals communicated to them via the media, a great number of individuals actually seek out idealized images in the media. Finally, we review what is known about the role of social media in impacting society’s perception of beauty and notions of idealized physical forms. Social media are more interactive than traditional media and the effects of self‐presentation strategies on perceptions of beauty have just begun to be studied. This is an emerging area of research that is of high relevance to researchers and clinicians interested in body image and appearance concerns.",book:{id:"5925",slug:"perception-of-beauty",title:"Perception of Beauty",fullTitle:"Perception of Beauty"},signatures:"Jennifer S. Mills, Amy Shannon and Jacqueline Hogue",authors:[{id:"202110",title:"Dr.",name:"Jennifer S.",middleName:null,surname:"Mills",slug:"jennifer-s.-mills",fullName:"Jennifer S. Mills"}]},{id:"59227",doi:"10.5772/intechopen.73385",title:"Differentiating Normal Cognitive Aging from Cognitive Impairment No Dementia: A Focus on Constructive and Visuospatial Abilities",slug:"differentiating-normal-cognitive-aging-from-cognitive-impairment-no-dementia-a-focus-on-constructive",totalDownloads:1353,totalCrossrefCites:3,totalDimensionsCites:6,abstract:"Constructive and visuospatial abilities in normal and in pathological aging (cognitive impairment, no dementia, CIND) are investigated. The sample includes 188 participants over 60 years of age, divided in 2 groups: healthy subjects (MMSE ≥28), without cognitive complaints, and individuals with CIND (MMSE between 24 and 27 and subjective cognitive complains). Drawing of cube and drawing of house, Benton Visual Retention Test (BVRT), and Block design are used to test the hypothesis that short visuoconstructive and visuospatial tests can distinguish normal from pathological cognitive aging in its very early stages. Results proved the discriminative sensitivity of BVRT general assessment criteria and of omissions and distortions in CIND. The diagnostic sensitivity of a modification of Moore and Wike [1984] scoring system for house and cube drawing tasks was confirmed as well. Drawing of cube and house could be used for quick screening of CIND in subjects over 60. Principal component analysis with oblimin rotation was performed to explore the different dimensions in the visuospatial and visuoconstructive abilities in old age. A four-factor structure was established, all four factors explaining 71% of the variance.",book:{id:"6381",slug:"gerontology",title:"Gerontology",fullTitle:"Gerontology"},signatures:"Radka Ivanova Massaldjieva",authors:[{id:"75907",title:"Associate Prof.",name:"Radka Ivanova",middleName:null,surname:"Massaldjieva",slug:"radka-ivanova-massaldjieva",fullName:"Radka Ivanova Massaldjieva"}]},{id:"59658",doi:"10.5772/intechopen.74748",title:"Ageing Better in the Netherlands",slug:"ageing-better-in-the-netherlands",totalDownloads:1193,totalCrossrefCites:1,totalDimensionsCites:4,abstract:"The Dutch National Care for the Elderly Programme was an initiative organized by the Netherlands Organisation for Health Research and Development (ZonMw) between 2008 and 2016. The aim of the programme was to collect knowledge about frail elderly, to assess their needs and to provide person-centred and integrated care better suited to their needs. The budget of EUR 88 million was provided by the Dutch Ministry of Health, Welfare and Sports. Putting the needs of elderly people at the heart of the programme and ensuring their active participation were key to the programme’s success. The programme outcomes included the establishment of eight geriatric networks around the medical universities with 650 organisations and the completion of 218 projects. These projects, involving 43,000 elderly people and 8500 central caregivers, resulted in the completion of 45 PhD theses and the publication of more than 400 articles and the development of 300 practice toolkits, one database and a website, www.beteroud.nl. The Dutch National Care for the Elderly Programme has since developed into a movement and continues under the consortium Ageing Better, made up of eight organisations. Through the use of ambassadors, Ageing Better promotes the message that ageing is not a disease but a new phase of life.",book:{id:"6381",slug:"gerontology",title:"Gerontology",fullTitle:"Gerontology"},signatures:"Betty Meyboom-de Jong, Klaske Wynia and Anjo Geluk-Bleumink",authors:[{id:"224997",title:"Emeritus Prof.",name:"Betty",middleName:null,surname:"Meyboom-De Jong",slug:"betty-meyboom-de-jong",fullName:"Betty Meyboom-De Jong"},{id:"232900",title:"Dr.",name:"Klaske",middleName:null,surname:"Wynia",slug:"klaske-wynia",fullName:"Klaske Wynia"},{id:"232901",title:"Mrs.",name:"Anjo",middleName:null,surname:"Geluk-Bleumink",slug:"anjo-geluk-bleumink",fullName:"Anjo Geluk-Bleumink"}]},{id:"55890",doi:"10.5772/intechopen.69529",title:"Mindfulness Meditation and the Perception of Beauty: Implications for an Ecological Well-Being",slug:"mindfulness-meditation-and-the-perception-of-beauty-implications-for-an-ecological-well-being",totalDownloads:1428,totalCrossrefCites:2,totalDimensionsCites:3,abstract:"Meditation is a first-person method for contemplating ourselves and the world, with more than 2500 years of history, rooted in the philosophical and contemplative traditions of the east. The present chapter aims to explore this worldview in order to demonstrate its relevance to our capacity for the appreciation of beauty. To this end, the aesthetic experience, the contemplative experience and their relationship with the practice of mindfulness are analysed. We suggest that the contemplative meditative experience bestows a state of consciousness and acceptance of life which places the practitioner in a progressive encounter with a self-concept that begins to detach from a static sense of the self and from the categories that define it, so that it may be experienced as an ongoing mental event, removed from cultural ideals of beauty or positivity. The result of this de-identification from the static self is a greater degree of psychological flexibility and a more genuine way of seeing the world, leading to a new perception of the self that is connected to an experience of freedom, and contributes to one’s own well-being, as well as to that of others and of the environment.",book:{id:"5925",slug:"perception-of-beauty",title:"Perception of Beauty",fullTitle:"Perception of Beauty"},signatures:"Álvaro I. Langer, Carlos Schmidt and Edwin Krogh",authors:[{id:"199843",title:"Dr.",name:"Álvaro",middleName:null,surname:"Langer",slug:"alvaro-langer",fullName:"Álvaro Langer"},{id:"201865",title:"MSc.",name:"Carlos",middleName:null,surname:"Schmidt",slug:"carlos-schmidt",fullName:"Carlos Schmidt"},{id:"201866",title:"Dr.",name:"Edwin",middleName:null,surname:"Krogh",slug:"edwin-krogh",fullName:"Edwin Krogh"}]}],mostDownloadedChaptersLast30Days:[{id:"60564",title:"Ageing Process and Physiological Changes",slug:"ageing-process-and-physiological-changes",totalDownloads:6996,totalCrossrefCites:19,totalDimensionsCites:34,abstract:"Ageing is a natural process. Everyone must undergo this phase of life at his or her own time and pace. In the broader sense, ageing reflects all the changes taking place over the course of life. These changes start from birth—one grows, develops and attains maturity. To the young, ageing is exciting. Middle age is the time when people notice the age-related changes like greying of hair, wrinkled skin and a fair amount of physical decline. Even the healthiest, aesthetically fit cannot escape these changes. Slow and steady physical impairment and functional disability are noticed resulting in increased dependency in the period of old age. According to World Health Organization, ageing is a course of biological reality which starts at conception and ends with death. It has its own dynamics, much beyond human control. However, this process of ageing is also subject to the constructions by which each society makes sense of old age. In most of the developed countries, the age of 60 is considered equivalent to retirement age and it is said to be the beginning of old age. In this chapter, you understand the details of ageing processes and associated physiological changes.",book:{id:"6381",slug:"gerontology",title:"Gerontology",fullTitle:"Gerontology"},signatures:"Shilpa Amarya, Kalyani Singh and Manisha Sabharwal",authors:[{id:"226573",title:"Ph.D.",name:"Shilpa",middleName:null,surname:"Amarya",slug:"shilpa-amarya",fullName:"Shilpa Amarya"},{id:"226593",title:"Dr.",name:"Kalyani",middleName:null,surname:"Singh",slug:"kalyani-singh",fullName:"Kalyani Singh"},{id:"243264",title:"Dr.",name:"Manisha",middleName:null,surname:"Sabharwal",slug:"manisha-sabharwal",fullName:"Manisha Sabharwal"}]},{id:"55388",title:"Beauty, Body Image, and the Media",slug:"beauty-body-image-and-the-media",totalDownloads:7764,totalCrossrefCites:5,totalDimensionsCites:12,abstract:"This chapter analyses the role of the mass media in people’s perceptions of beauty. We summarize the research literature on the mass media, both traditional media and online social media, and how they appear to interact with psychological factors to impact appearance concerns and body image disturbances. There is a strong support for the idea that traditional forms of media (e.g. magazines and music videos) affect perceptions of beauty and appearance concerns by leading women to internalize a very slender body type as ideal or beautiful. Rather than simply being passive recipients of unrealistic beauty ideals communicated to them via the media, a great number of individuals actually seek out idealized images in the media. Finally, we review what is known about the role of social media in impacting society’s perception of beauty and notions of idealized physical forms. Social media are more interactive than traditional media and the effects of self‐presentation strategies on perceptions of beauty have just begun to be studied. This is an emerging area of research that is of high relevance to researchers and clinicians interested in body image and appearance concerns.",book:{id:"5925",slug:"perception-of-beauty",title:"Perception of Beauty",fullTitle:"Perception of Beauty"},signatures:"Jennifer S. Mills, Amy Shannon and Jacqueline Hogue",authors:[{id:"202110",title:"Dr.",name:"Jennifer S.",middleName:null,surname:"Mills",slug:"jennifer-s.-mills",fullName:"Jennifer S. Mills"}]},{id:"56505",title:"Aesthetics of the Naked Human Body: From Pornography (Sexualised Lust Object) to Iconography (Aesthetics of Human Nobility and Wisdom) in an Anthropology of Physical Beauty",slug:"aesthetics-of-the-naked-human-body-from-pornography-sexualised-lust-object-to-iconography-aesthetics",totalDownloads:2100,totalCrossrefCites:0,totalDimensionsCites:0,abstract:"In many religious circles and philosophies of life, the human body is excluded from the realm of spirituality and meaning. Due to a dualistic approach, nudity is viewed as merely a physical and corporeal category. In social media, there is the real danger that the naked human body is exploited for commercial gain. Advertisements often leave the impression that the body, very specifically the genitals, is designed merely for physical desire and corporeal chemistry. They become easily objects for lust, excluded from the beauty of graceful existence and noble courage. It is argued that the naked human body is not designed for pornographic exploitation and promiscuous sensuality but for compassionate intimacy and nurturing care in order to instil a humane dimension in human and sexual encounters. In this regard, antiquity and the Michelangelesque perspective can contribute to a paradigm shift from abusive exploitation to the beauty of vulnerable sensitivity. In order to foster an integrative approach to theory formation in anthropology, the methodology of stereometric thinking is proposed.",book:{id:"5925",slug:"perception-of-beauty",title:"Perception of Beauty",fullTitle:"Perception of Beauty"},signatures:"Daniel J Louw",authors:[{id:"200645",title:"Prof.",name:"Daniel",middleName:"Johannes",surname:"Louw",slug:"daniel-louw",fullName:"Daniel Louw"}]},{id:"56059",title:"A Plastic Surgeon’s Perspective on Stereotyping and the Perception of Beauty",slug:"a-plastic-surgeon-s-perspective-on-stereotyping-and-the-perception-of-beauty",totalDownloads:1918,totalCrossrefCites:0,totalDimensionsCites:1,abstract:"In the world of plastic surgery, misconceptions may lead to irrational requests or outcomes not appreciated by patients. Those who manage aesthetics should always listen and recognize the variability of cultural identities, desires, attitudes, anxieties and uncertainties of the patient. Emerging from a diversity of cultures and its transforming trends, the scope of cosmetic surgery and its practice reflect not only the individual’s personality, but also the culture as a whole. When counseling an individual, one has to recognize that even in groups of seemingly identical social or cultural standards; there are subtle differences in expectations. To illustrate the potential for inaccuracy of ethnic profiling in the field of plastic surgery authors quote their own work on Asian subjects and facial beauty and resort to experience of others. To reaffirm their opinion and to exemplify how sometimes “fine” differences in the perception of beauty exist, an original study that evaluates the preferences among selected groups of Latina women in respect to buttock aesthetics has been included. This dissertation will focus on how cultural factors influence beauty perception; strengthen the fact that beauty is in the eye of the beholder and how variable differences exist even between small subgroups.",book:{id:"5925",slug:"perception-of-beauty",title:"Perception of Beauty",fullTitle:"Perception of Beauty"},signatures:"Johanna D’Agostino and Marek Dobke",authors:[{id:"17590",title:"Dr.",name:"Marek K.",middleName:null,surname:"Dobke",slug:"marek-k.-dobke",fullName:"Marek K. Dobke"},{id:"201244",title:"Dr.",name:"Johanna",middleName:null,surname:"D'Agostino",slug:"johanna-d'agostino",fullName:"Johanna D'Agostino"}]},{id:"80326",title:"Anti-Senescence Therapy",slug:"anti-senescence-therapy",totalDownloads:110,totalCrossrefCites:0,totalDimensionsCites:0,abstract:"The development of therapeutic strategies aimed at the aging process of cells has attracted increasing attention in recent decades due to the involvement of this process in the development of many chronic and age-related diseases. Interestingly, preclinical studies have shown the success of a number of anti-aging approaches in the treatment of a range of chronic diseases. These approaches are directed against aging processes such as oxidative stress, telomerase shortening, inflammation, and deficient autophagy. Many strategies has been shown to be effective in delaying aging, including antiaging strategies based on establishing healthy lifestyle habits and pharmacological interventions aimed at disrupting senescent cells and senescent-associated secretory phenotype. Caloric restriction and intermittent fasting were reported to activate autophagy and reduce inflammation. In turn, immune-based strategies, senolytic agents, and senomorphics mediate their effects either by eliminating senescent cells through inducing apoptosis or by disrupting pathways by which senescent cells mediate their detrimental effects. In addition, given the association of the decline in the regenerative potential of stem cells with aging, many experimental and clinical studies indicate the effectiveness of stem cell transplantation in preventing or slowing the progress of age-related diseases by enhancing the repairing mechanisms and the secretion of many growth factors and cytokines.",book:{id:"10935",slug:null,title:"Mechanisms and Management of Senescence",fullTitle:"Mechanisms and Management of Senescence"},signatures:"Raghad Alshadidi",authors:null}],onlineFirstChaptersFilter:{topicId:"235",limit:6,offset:0},onlineFirstChaptersCollection:[{id:"82112",title:"Comparative Senescence and Lifespan",slug:"comparative-senescence-and-lifespan",totalDownloads:17,totalDimensionsCites:0,doi:"10.5772/intechopen.105137",abstract:"The word senescence is derived from the Latin word “senex” (meaning old). In biology, senescence is a process by which a cell ages and permanently stops dividing. Senescence is a natural universal phenomenon affecting all living organisms (e.g., humans, animals, and plants). It is the process of growing old (aging). The underlying mechanisms of senescence and aging at the cellular level are not fully understood. Senescence is a multifactorial process that can be induced by several stimuli including cellular stress, DNA damage, telomere shortening, and oncogene activation. The most popular theory to explain aging is the free radical theory. Senescence plays a role in the development of several age-related chronic diseases in humans (e.g., ischemic heart disease, osteoporosis, and cancer). Lifespan is a biological characteristic of every species. The lifespan of living organisms ranges from few hours (with mayfly) to potential eternity (with jellyfish and hydra). The maximum theoretical lifespan in humans is around 120 years. The lifespan in humans is influenced by multiple factors including genetic, epigenetic, lifestyle, environmental, metabolic, and endocrine factors. There are several ways to potentially extend the lifespan of humans and eventually surpass the maximum theoretical lifespan of 120 years. The tools that can be proposed include lifestyle, reduction of several life-threatening diseases and disabilities, hormonal replacement, antioxidants, autophagy inducers, senolytic drugs, stem cell therapy, and gene therapy.",book:{id:"10935",title:"Mechanisms and Management of Senescence",coverURL:"https://cdn.intechopen.com/books/images_new/10935.jpg"},signatures:"Hassan M. Heshmati"},{id:"81638",title:"Aging and Neuropsychiatric Disease: A General Overview of Prevalence and Trends",slug:"aging-and-neuropsychiatric-disease-a-general-overview-of-prevalence-and-trends",totalDownloads:30,totalDimensionsCites:0,doi:"10.5772/intechopen.103102",abstract:"The increasing trend of life-expectancy is becoming a significant demographic, societal and economic challenge. Currently, global number of people above sixty years of age is 900 million, while United Nations expect this number to rise to over 1.4 billion in 2030 and over 2.5 billion by 2050. Concordant to this trend, numerous physiological changes are associated with aging and brain-related ones are associated with neuropsychiatric diseases. The main goal of this chapter is to identify the most important neuropsychiatric diseases to assess in older patients to help to promote health and prevent diseases and complications associated with chronic illness, as these changes are progressive and require important psychological and setting-related social adjustments. Findings identify several health-aspects highly present in elderly: stroke, white matter lesions, dementia rise with age, changes in levels of neurotransmitters and hormones, depression as well as the bereavement following loss of the loved one, and the most common neurodegenerative disease—Alzheimer’s disease and Parkinson’s. In conclusion, studying the aging process should include all developmental, circumstantial, and individual aspects of aging. This offers opportunities to improve the health of elderly by using a wide range of skills and knowledge. Thus, further studies are necessary to elucidate what can be done do to improve the aging process and health of elderly in the future.",book:{id:"10935",title:"Mechanisms and Management of Senescence",coverURL:"https://cdn.intechopen.com/books/images_new/10935.jpg"},signatures:"Jelena Milić"},{id:"80326",title:"Anti-Senescence Therapy",slug:"anti-senescence-therapy",totalDownloads:110,totalDimensionsCites:0,doi:"10.5772/intechopen.101585",abstract:"The development of therapeutic strategies aimed at the aging process of cells has attracted increasing attention in recent decades due to the involvement of this process in the development of many chronic and age-related diseases. Interestingly, preclinical studies have shown the success of a number of anti-aging approaches in the treatment of a range of chronic diseases. These approaches are directed against aging processes such as oxidative stress, telomerase shortening, inflammation, and deficient autophagy. Many strategies has been shown to be effective in delaying aging, including antiaging strategies based on establishing healthy lifestyle habits and pharmacological interventions aimed at disrupting senescent cells and senescent-associated secretory phenotype. Caloric restriction and intermittent fasting were reported to activate autophagy and reduce inflammation. In turn, immune-based strategies, senolytic agents, and senomorphics mediate their effects either by eliminating senescent cells through inducing apoptosis or by disrupting pathways by which senescent cells mediate their detrimental effects. In addition, given the association of the decline in the regenerative potential of stem cells with aging, many experimental and clinical studies indicate the effectiveness of stem cell transplantation in preventing or slowing the progress of age-related diseases by enhancing the repairing mechanisms and the secretion of many growth factors and cytokines.",book:{id:"10935",title:"Mechanisms and Management of Senescence",coverURL:"https://cdn.intechopen.com/books/images_new/10935.jpg"},signatures:"Raghad Alshadidi"},{id:"79828",title:"Cellular Senescence in Bone",slug:"cellular-senescence-in-bone",totalDownloads:119,totalDimensionsCites:0,doi:"10.5772/intechopen.101803",abstract:"Senescence is an irreversible cell-cycle arrest process induced by environmental, genetic, and epigenetic factors. An accumulation of senescent cells in bone results in age-related disorders, and one of the common problems is osteoporosis. Deciphering the basic mechanisms contributing to the chronic ailments of aging may uncover new avenues for targeted treatment. This review focuses on the mechanisms and the most relevant research advancements in skeletal cellular senescence. To identify new options for the treatment or prevention of age-related chronic diseases, researchers have targeted hallmarks of aging, including telomere attrition, genomic instability, cellular senescence, and epigenetic alterations. First, this chapter provides an overview of the fundamentals of bone tissue, the causes of skeletal involution, and the role of cellular senescence in bone and bone diseases such as osteoporosis. Next, this review will discuss the utilization of pharmacological interventions in aging tissues and, more specifically, highlight the role of senescent cells to identify the most effective and safe strategies.",book:{id:"10935",title:"Mechanisms and Management of Senescence",coverURL:"https://cdn.intechopen.com/books/images_new/10935.jpg"},signatures:"Danielle Wang and Haitao Wang"},{id:"79668",title:"Identification of RNA Species That Bind to the hnRNP A1 in Normal and Senescent Human Fibroblasts",slug:"identification-of-rna-species-that-bind-to-the-hnrnp-a1-in-normal-and-senescent-human-fibroblasts",totalDownloads:81,totalDimensionsCites:0,doi:"10.5772/intechopen.101525",abstract:"hnRNP A1 is a member of the hnRNPs (heterogeneous nuclear ribonucleoproteins) family of proteins that play a central role in regulating genes responsible for cell proliferation, DNA repair, apoptosis, and telomere biogenesis. Previous studies have shown that hnRNPA1 had reduced protein levels and increased cytoplasmic accumulation in senescent human diploid fibroblasts. The consequence of reduced protein expression and altered cellular localization may account for the alterations in gene expression observed during senescence. There is limited information for gene targets of hnRNP A1 as well as its in vivo function. In these studies, we performed RNA co-immunoprecipitation experiments using hnRNP A1 as the target protein to identify potential mRNA species in ribonucleoprotein (RNP) complexes. Using this approach, we identified the human double minute 2 (HDM2) mRNA as a binding target for hnRNP A1 in young and senescent human diploid fibroblasts cells. It was also observed that alterations of hnRNP A1 expression modulate HDM2 mRNA levels in young IMR-90 cells. We also demonstrated that the levels of HDM2 mRNA increased with the downregulation of hnRNP A1 and decrease with the overexpression of hnRNP A1. Although we did not observe a significant decrease in HDM2 protein level, a concomitant increase in p53 protein level was detected with the overexpression of hnRNP A1. Our studies also show that hnRNP A1 directly interacts with HDM2 mRNA at a region corresponding to its 3′ UTR (untranslated region of a gene). The results from this study demonstrate that hnRNP A1 has a novel role in participating in the regulation of HDM2 gene expression.",book:{id:"10935",title:"Mechanisms and Management of Senescence",coverURL:"https://cdn.intechopen.com/books/images_new/10935.jpg"},signatures:"Heriberto Moran, Shanaz A. Ghandhi, Naoko Shimada and Karen Hubbard"},{id:"79295",title:"Genetic and Epigenetic Influences on Cutaneous Cellular Senescence",slug:"genetic-and-epigenetic-influences-on-cutaneous-cellular-senescence",totalDownloads:135,totalDimensionsCites:0,doi:"10.5772/intechopen.101152",abstract:"Skin is the largest human organ system, and its protective function is critical to survival. The epithelial, dermal, and subcutaneous compartments are heterogeneous mixtures of cell types, yet they all display age-related skin dysfunction through the accumulation of an altered phenotypic cellular state called senescence. Cellular senescence is triggered by complex and dynamic genetic and epigenetic processes. A senescence steady state is achieved in different cell types under various and overlapping conditions of chronological age, toxic injury, oxidative stress, replicative exhaustion, DNA damage, metabolic dysfunction, and chromosomal structural changes. These inputs lead to outputs of cell-cycle withdrawal and the appearance of a senescence-associated secretory phenotype, both of which accumulate as tissue pathology observed clinically in aged skin. This review details the influence of genetic and epigenetic factors that converge on normal cutaneous cellular processes to create the senescent state, thereby dictating the response of the skin to the forces of both intrinsic and extrinsic aging. From this work, it is clear that no single biomarker or process leads to senescence, but that it is a convergence of factors resulting in an overt aging phenotype.",book:{id:"10935",title:"Mechanisms and Management of Senescence",coverURL:"https://cdn.intechopen.com/books/images_new/10935.jpg"},signatures:"Tapash Jay Sarkar, Maiko Hermsmeier, Jessica L. Ross and G. Scott Herron"}],onlineFirstChaptersTotal:6},preDownload:{success:null,errors:{}},subscriptionForm:{success:null,errors:{}},aboutIntechopen:{},privacyPolicy:{},peerReviewing:{},howOpenAccessPublishingWithIntechopenWorks:{},sponsorshipBooks:{sponsorshipBooks:[],offset:8,limit:8,total:0},allSeries:{pteSeriesList:[{id:"14",title:"Artificial Intelligence",numberOfPublishedBooks:9,numberOfPublishedChapters:90,numberOfOpenTopics:6,numberOfUpcomingTopics:0,issn:"2633-1403",doi:"10.5772/intechopen.79920",isOpenForSubmission:!0},{id:"7",title:"Biomedical Engineering",numberOfPublishedBooks:12,numberOfPublishedChapters:107,numberOfOpenTopics:3,numberOfUpcomingTopics:0,issn:"2631-5343",doi:"10.5772/intechopen.71985",isOpenForSubmission:!0}],lsSeriesList:[{id:"11",title:"Biochemistry",numberOfPublishedBooks:33,numberOfPublishedChapters:330,numberOfOpenTopics:4,numberOfUpcomingTopics:0,issn:"2632-0983",doi:"10.5772/intechopen.72877",isOpenForSubmission:!0},{id:"25",title:"Environmental Sciences",numberOfPublishedBooks:1,numberOfPublishedChapters:19,numberOfOpenTopics:4,numberOfUpcomingTopics:0,issn:"2754-6713",doi:"10.5772/intechopen.100362",isOpenForSubmission:!0},{id:"10",title:"Physiology",numberOfPublishedBooks:14,numberOfPublishedChapters:145,numberOfOpenTopics:4,numberOfUpcomingTopics:0,issn:"2631-8261",doi:"10.5772/intechopen.72796",isOpenForSubmission:!0}],hsSeriesList:[{id:"3",title:"Dentistry",numberOfPublishedBooks:9,numberOfPublishedChapters:140,numberOfOpenTopics:2,numberOfUpcomingTopics:0,issn:"2631-6218",doi:"10.5772/intechopen.71199",isOpenForSubmission:!0},{id:"6",title:"Infectious Diseases",numberOfPublishedBooks:13,numberOfPublishedChapters:123,numberOfOpenTopics:4,numberOfUpcomingTopics:0,issn:"2631-6188",doi:"10.5772/intechopen.71852",isOpenForSubmission:!0},{id:"13",title:"Veterinary Medicine and Science",numberOfPublishedBooks:11,numberOfPublishedChapters:112,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:22,numberOfOpenTopics:3,numberOfUpcomingTopics:0,issn:"2753-894X",doi:"10.5772/intechopen.100359",isOpenForSubmission:!0},{id:"23",title:"Education and Human Development",numberOfPublishedBooks:0,numberOfPublishedChapters:11,numberOfOpenTopics:1,numberOfUpcomingTopics:1,issn:null,doi:"10.5772/intechopen.100360",isOpenForSubmission:!0},{id:"24",title:"Sustainable Development",numberOfPublishedBooks:1,numberOfPublishedChapters:19,numberOfOpenTopics:5,numberOfUpcomingTopics:0,issn:"2753-6580",doi:"10.5772/intechopen.100361",isOpenForSubmission:!0}],testimonialsList:[{id:"13",text:"The collaboration with and support of the technical staff of IntechOpen is fantastic. 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This series is intended for doctors, engineers, and scientists involved in biomedical engineering or those wanting to start working in this field.",coverUrl:"https://cdn.intechopen.com/series/covers/7.jpg",latestPublicationDate:"August 3rd, 2022",hasOnlineFirst:!0,numberOfOpenTopics:3,numberOfPublishedChapters:107,numberOfPublishedBooks:12,editor:{id:"50150",title:"Prof.",name:"Robert",middleName:null,surname:"Koprowski",fullName:"Robert Koprowski",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002aYTYNQA4/Profile_Picture_1630478535317",biography:"Robert Koprowski, MD (1997), PhD (2003), Habilitation (2015), is an employee of the University of Silesia, Poland, Institute of Computer Science, Department of Biomedical Computer Systems. For 20 years, he has studied the analysis and processing of biomedical images, emphasizing the full automation of measurement for a large inter-individual variability of patients. Dr. Koprowski has authored more than a hundred research papers with dozens in impact factor (IF) journals and has authored or co-authored six books. Additionally, he is the author of several national and international patents in the field of biomedical devices and imaging. Since 2011, he has been a reviewer of grants and projects (including EU projects) in biomedical engineering.",institutionString:null,institution:{name:"University of Silesia",institutionURL:null,country:{name:"Poland"}}},subseries:[{id:"7",title:"Bioinformatics and Medical Informatics",keywords:"Biomedical Data, Drug Discovery, Clinical Diagnostics, Decoding Human Genome, AI in Personalized Medicine, Disease-prevention Strategies, Big Data Analysis in Medicine",scope:"Bioinformatics aims to help understand the functioning of the mechanisms of living organisms through the construction and use of quantitative tools. The applications of this research cover many related fields, such as biotechnology and medicine, where, for example, Bioinformatics contributes to faster drug design, DNA analysis in forensics, and DNA sequence analysis in the field of personalized medicine. Personalized medicine is a type of medical care in which treatment is customized individually for each patient. Personalized medicine enables more effective therapy, reduces the costs of therapy and clinical trials, and also minimizes the risk of side effects. Nevertheless, advances in personalized medicine would not have been possible without bioinformatics, which can analyze the human genome and other vast amounts of biomedical data, especially in genetics. The rapid growth of information technology enabled the development of new tools to decode human genomes, large-scale studies of genetic variations and medical informatics. The considerable development of technology, including the computing power of computers, is also conducive to the development of bioinformatics, including personalized medicine. In an era of rapidly growing data volumes and ever lower costs of generating, storing and computing data, personalized medicine holds great promises. Modern computational methods used as bioinformatics tools can integrate multi-scale, multi-modal and longitudinal patient data to create even more effective and safer therapy and disease prevention methods. Main aspects of the topic are: Applying bioinformatics in drug discovery and development; Bioinformatics in clinical diagnostics (genetic variants that act as markers for a condition or a disease); Blockchain and Artificial Intelligence/Machine Learning in personalized medicine; Customize disease-prevention strategies in personalized medicine; Big data analysis in personalized medicine; Translating stratification algorithms into clinical practice of personalized medicine.",annualVolume:11403,isOpenForSubmission:!0,coverUrl:"https://cdn.intechopen.com/series_topics/covers/7.jpg",editor:{id:"351533",title:"Dr.",name:"Slawomir",middleName:null,surname:"Wilczynski",fullName:"Slawomir Wilczynski",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0033Y000035U1loQAC/Profile_Picture_1630074514792",institutionString:null,institution:{name:"Medical University of Silesia",institutionURL:null,country:{name:"Poland"}}},editorTwo:null,editorThree:null,editorialBoard:[{id:"5886",title:"Dr.",name:"Alexandros",middleName:"T.",surname:"Tzallas",fullName:"Alexandros Tzallas",profilePictureURL:"https://mts.intechopen.com/storage/users/5886/images/system/5886.png",institutionString:"University of Ioannina, Greece & Imperial College London",institution:{name:"University of Ioannina",institutionURL:null,country:{name:"Greece"}}},{id:"257388",title:"Distinguished Prof.",name:"Lulu",middleName:null,surname:"Wang",fullName:"Lulu Wang",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bRX6kQAG/Profile_Picture_1630329584194",institutionString:"Shenzhen Technology University",institution:{name:"Shenzhen Technology University",institutionURL:null,country:{name:"China"}}},{id:"225387",title:"Prof.",name:"Reda R.",middleName:"R.",surname:"Gharieb",fullName:"Reda R. Gharieb",profilePictureURL:"https://mts.intechopen.com/storage/users/225387/images/system/225387.jpg",institutionString:"Assiut University",institution:{name:"Assiut University",institutionURL:null,country:{name:"Egypt"}}}]},{id:"8",title:"Bioinspired Technology and Biomechanics",keywords:"Bioinspired Systems, Biomechanics, Assistive Technology, Rehabilitation",scope:'Bioinspired technologies take advantage of understanding the actual biological system to provide solutions to problems in several areas. Recently, bioinspired systems have been successfully employing biomechanics to develop and improve assistive technology and rehabilitation devices. The research topic "Bioinspired Technology and Biomechanics" welcomes studies reporting recent advances in bioinspired technologies that contribute to individuals\' health, inclusion, and rehabilitation. Possible contributions can address (but are not limited to) the following research topics: Bioinspired design and control of exoskeletons, orthoses, and prostheses; Experimental evaluation of the effect of assistive devices (e.g., influence on gait, balance, and neuromuscular system); Bioinspired technologies for rehabilitation, including clinical studies reporting evaluations; Application of neuromuscular and biomechanical models to the development of bioinspired technology.',annualVolume:11404,isOpenForSubmission:!0,coverUrl:"https://cdn.intechopen.com/series_topics/covers/8.jpg",editor:{id:"144937",title:"Prof.",name:"Adriano",middleName:"De Oliveira",surname:"Andrade",fullName:"Adriano Andrade",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bRC8QQAW/Profile_Picture_1625219101815",institutionString:null,institution:{name:"Federal University of Uberlândia",institutionURL:null,country:{name:"Brazil"}}},editorTwo:null,editorThree:null,editorialBoard:[{id:"49517",title:"Prof.",name:"Hitoshi",middleName:null,surname:"Tsunashima",fullName:"Hitoshi Tsunashima",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002aYTP4QAO/Profile_Picture_1625819726528",institutionString:null,institution:{name:"Nihon University",institutionURL:null,country:{name:"Japan"}}},{id:"425354",title:"Dr.",name:"Marcus",middleName:"Fraga",surname:"Vieira",fullName:"Marcus Vieira",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0033Y00003BJSgIQAX/Profile_Picture_1627904687309",institutionString:null,institution:{name:"Universidade Federal de Goiás",institutionURL:null,country:{name:"Brazil"}}},{id:"196746",title:"Dr.",name:"Ramana",middleName:null,surname:"Vinjamuri",fullName:"Ramana Vinjamuri",profilePictureURL:"https://mts.intechopen.com/storage/users/196746/images/system/196746.jpeg",institutionString:"University of Maryland, Baltimore County",institution:{name:"University of Maryland, Baltimore County",institutionURL:null,country:{name:"United States of America"}}}]},{id:"9",title:"Biotechnology - Biosensors, Biomaterials and Tissue Engineering",keywords:"Biotechnology, Biosensors, Biomaterials, Tissue Engineering",scope:"The Biotechnology - Biosensors, Biomaterials and Tissue Engineering topic within the Biomedical Engineering Series aims to rapidly publish contributions on all aspects of biotechnology, biosensors, biomaterial and tissue engineering. We encourage the submission of manuscripts that provide novel and mechanistic insights that report significant advances in the fields. Topics can include but are not limited to: Biotechnology such as biotechnological products and process engineering; Biotechnologically relevant enzymes and proteins; Bioenergy and biofuels; Applied genetics and molecular biotechnology; Genomics, transcriptomics, proteomics; Applied microbial and cell physiology; Environmental biotechnology; Methods and protocols. Moreover, topics in biosensor technology, like sensors that incorporate enzymes, antibodies, nucleic acids, whole cells, tissues and organelles, and other biological or biologically inspired components will be considered, and topics exploring transducers, including those based on electrochemical and optical piezoelectric, thermal, magnetic, and micromechanical elements. Chapters exploring biomaterial approaches such as polymer synthesis and characterization, drug and gene vector design, biocompatibility, immunology and toxicology, and self-assembly at the nanoscale, are welcome. Finally, the tissue engineering subcategory will support topics such as the fundamentals of stem cells and progenitor cells and their proliferation, differentiation, bioreactors for three-dimensional culture and studies of phenotypic changes, stem and progenitor cells, both short and long term, ex vivo and in vivo implantation both in preclinical models and also in clinical trials.",annualVolume:11405,isOpenForSubmission:!0,coverUrl:"https://cdn.intechopen.com/series_topics/covers/9.jpg",editor:{id:"126286",title:"Dr.",name:"Luis",middleName:"Jesús",surname:"Villarreal-Gómez",fullName:"Luis Villarreal-Gómez",profilePictureURL:"https://mts.intechopen.com/storage/users/126286/images/system/126286.jpg",institutionString:null,institution:{name:"Autonomous University of Baja California",institutionURL:null,country:{name:"Mexico"}}},editorTwo:null,editorThree:null,editorialBoard:[{id:"35539",title:"Dr.",name:"Cecilia",middleName:null,surname:"Cristea",fullName:"Cecilia Cristea",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002aYQ65QAG/Profile_Picture_1621007741527",institutionString:null,institution:{name:"Iuliu Hațieganu University of Medicine and Pharmacy",institutionURL:null,country:{name:"Romania"}}},{id:"40735",title:"Dr.",name:"Gil",middleName:"Alberto Batista",surname:"Gonçalves",fullName:"Gil Gonçalves",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002aYRLGQA4/Profile_Picture_1628492612759",institutionString:null,institution:{name:"University of Aveiro",institutionURL:null,country:{name:"Portugal"}}},{id:"211725",title:"Associate Prof.",name:"Johann F.",middleName:null,surname:"Osma",fullName:"Johann F. 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Valarmathi",profilePictureURL:"https://mts.intechopen.com/storage/users/69697/images/system/69697.jpg",institutionString:"Religen Inc. | A Life Science Company, United States of America",institution:null},{id:"205081",title:"Dr.",name:"Marco",middleName:"Vinícius",surname:"Chaud",fullName:"Marco Chaud",profilePictureURL:"https://s3.us-east-1.amazonaws.com/intech-files/0030O00002bSDGeQAO/Profile_Picture_1622624307737",institutionString:null,institution:{name:"Universidade de Sorocaba",institutionURL:null,country:{name:"Brazil"}}}]}]}},libraryRecommendation:{success:null,errors:{},institutions:[]},route:{name:"chapter.detail",path:"/chapters/39015",hash:"",query:{},params:{id:"39015"},fullPath:"/chapters/39015",meta:{},from:{name:null,path:"/",hash:"",query:{},params:{},fullPath:"/",meta:{}}}},function(){var t;(t=document.currentScript||document.scripts[document.scripts.length-1]).parentNode.removeChild(t)}()