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Type-1 Diabetes

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Cover of 'Type-1 Diabetes'

Table of Contents

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    Book Overview
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    Chapter 286 Methylation Analysis in Distinct Immune Cell Subsets in Type 1 Diabetes.
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    Chapter 287 Histology of Type 1 Diabetes Pancreas.
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    Chapter 288 Fluorescence In Situ Hybridization with Concomitant Immunofluorescence in Human Pancreas.
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    Chapter 289 Type 1 Diabetes: Current Perspectives.
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    Chapter 290 Laser Capture and Single Cell Genotyping from Frozen Tissue Sections.
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    Chapter 291 Pancreatic Beta Cell Survival and Signaling Pathways: Effects of Type 1 Diabetes-Associated Genetic Variants.
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    Chapter 292 Islet Autoantibody Analysis: Radioimmunoassays.
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    Chapter 293 Tracking Immunological Responses of Islet Antigen-Specific T Cells in the Nonobese Diabetic (NOD) Mouse Model of Type 1 Diabetes.
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    Chapter 294 Adoptive Transfer of Autoimmune Diabetes Using Immunodeficient Nonobese Diabetic (NOD) Mice.
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    Chapter 295 Identification of Islet Antigen-Specific CD8 T Cells Using MHCI-Peptide Tetramer Reagents in the Non Obese Diabetic (NOD) Mouse Model of Type 1 Diabetes.
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    Chapter 296 Islet Autoantibody Detection by Electrochemiluminescence (ECL) Assay.
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    Chapter 307 Type 1 Diabetes High-Risk HLA Class II Determination by Polymerase Chain Reaction Sequence-Specific Primers.
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    Chapter 330 Detection of C-Peptide in Urine as a Measure of Ongoing Beta Cell Function
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    Chapter 331 The Gut Microbiome in the NOD Mouse
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    Chapter 339 Molecular Methods and Protein Synthesis for Definition of Autoantibody Epitopes.
Attention for Chapter 287: Histology of Type 1 Diabetes Pancreas.
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Chapter title
Histology of Type 1 Diabetes Pancreas.
Chapter number 287
Book title
Type-1 Diabetes
Published in
Methods in molecular biology, January 2016
DOI 10.1007/7651_2015_287
Pubmed ID
Book ISBNs
978-1-4939-3641-0, 978-1-4939-3643-4
Authors

Abby Willcox, Kathleen M. Gillespie

Editors

Kathleen M. Gillespie

Abstract

The islets of Langerhans play a critical role in glucose homeostasis. Islets are predominantly composed of insulin-secreting beta cells and glucagon-secreting alpha cells. In type 1 diabetes, the beta cells are destroyed by autoimmune destruction of insulin producing beta cells resulting in hyperglycemia. This is a gradual process, taking from several months to decades. Much of the beta cell destruction takes place during a silent, asymptomatic phase. Type 1 diabetes becomes clinically evident upon destruction of approximately 70-80 % of beta cell mass. Studying the decline in beta cell mass and the cells which are responsible for their demise is difficult as pancreatic biopsies are not feasible in patients with type 1 diabetes. The relative size of islets and their dispersed location throughout the pancreas means in vivo imaging of human islets is currently not manageable. At present, there are no validated biomarkers which accurately track the decline in beta cell mass in individuals who are at risk of developing, or have already developed, type 1 diabetes. Therefore, studies of pancreatic tissue retrieved at autopsy from donors with type 1 diabetes, or donors with high risk markers of type 1 diabetes such as circulating islet-associated autoantibodies, is currently the best method for studying beta cells and the associated inflammatory milieu in situ. In recent years, concerted efforts have been made to source such tissues for histological studies, enabling great insights to be made into the relationship between islets and the inflammatory insult to which they are subjected. This article describes in detail, a robust immunohistochemical method which can be utilized to study both recent, and archival human pancreatic tissue, in order to examine islet endocrine cells and the surrounding immune cells.

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Mendeley readers

The data shown below were compiled from readership statistics for 48 Mendeley readers of this research output. Click here to see the associated Mendeley record.

Geographical breakdown

Country Count As %
Unknown 48 100%

Demographic breakdown

Readers by professional status Count As %
Student > Bachelor 14 29%
Student > Master 5 10%
Student > Postgraduate 5 10%
Student > Ph. D. Student 5 10%
Researcher 3 6%
Other 3 6%
Unknown 13 27%
Readers by discipline Count As %
Medicine and Dentistry 10 21%
Biochemistry, Genetics and Molecular Biology 9 19%
Engineering 4 8%
Agricultural and Biological Sciences 3 6%
Pharmacology, Toxicology and Pharmaceutical Science 3 6%
Other 6 13%
Unknown 13 27%