Dimorphic histopathology of long-standing childhood-onset diabetes

Aims/hypothesis Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells. Analysis of C-peptide in children characterised at diabetes onset for autoantibodies shows heterogeneous preservation of insulin secretion in long-s...

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Published in:	Diabetologia Vol. 53; no. 4; pp. 690 - 698
Main Authors:	Gianani, R, Campbell-Thompson, M, Sarkar, S. A, Wasserfall, C, Pugliese, A, Solis, J. M, Kent, S. C, Hering, B. J, West, E, Steck, A, Bonner-Weir, S, Atkinson, M. A, Coppieters, K, von Herrath, M, Eisenbarth, G. S
Format:	Journal Article
Language:	English
Published:	Berlin/Heidelberg Berlin/Heidelberg : Springer-Verlag 01.04.2010 Springer-Verlag Springer Springer Nature B.V
Subjects:	Adolescent Adult African Americans Age of Onset Apoptosis Autoantibodies Autoantibodies - blood Autoimmune diabetes Autopsies Biological and medical sciences blood C-Peptide C-Peptide - blood Child Child, Preschool Childhood diabetes Diabetes Diabetes Mellitus, Type 1 Diabetes Mellitus, Type 1 - immunology Diabetes Mellitus, Type 1 - pathology Diabetes. Impaired glucose tolerance Endocrine pancreas. Apud cells (diseases) Endocrinopathies Etiopathogenesis. Screening. Investigations. Target tissue resistance Female Heterogeneity of diabetes Hispanic people Histocompatibility Testing Histopathology HLA DR3 HLA DR4 HLA-DR Antigens Human Physiology Humans Hyperinsulinism Hyperinsulinism - pathology immunology Insulin insulin-dependent diabetes mellitus Insulin-Secreting Cells Insulin-Secreting Cells - pathology Internal Medicine Islet autoantibodies Male Medical sciences Medicine Medicine & Public Health Metabolic Diseases Middle Aged Organ donors Pancreas Pancreas - pathology Pathology Pathology of childhood diabetes Patterns of beta cell loss Peptides Sex Characteristics Tissue Donors United States > US Islet autoantibodies Childhood diabetes Type 1 diabetes HLA DR3 HLA DR4 Autoimmune diabetes Patterns of beta cell loss Pathology of childhood diabetes Heterogeneity of diabetes Organ donors Endocrinopathy Autoimmunity Immunopathology HLA-System Langerhans islet Autoantibody Autoimmune disease Anatomic pathology Histopathology Donor β Cell Endocrine pancreas
ISSN:	0012-186X, 1432-0428, 1432-0428
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Abstract	Aims/hypothesis Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells. Analysis of C-peptide in children characterised at diabetes onset for autoantibodies shows heterogeneous preservation of insulin secretion in long-standing diabetes. The aim of this study was to characterise the pancreases of childhood-onset diabetes in order to define the pathological basis of this heterogeneity. Methods We evaluated 20 cadaveric organ donor pancreases of childhood-onset long-term patients for disease heterogeneity and obtained corresponding C-peptide measurements. Results Pancreases from the majority of cadaveric donors contained only insulin-deficient islets (14 of 20). The remaining six patients (30%) had numerous insulin-positive cells within at least some islets, with two different histological patterns. Pattern A (which we would associate with type 1A diabetes) had lobular retention of areas with ‘abnormal' beta cells producing the apoptosis inhibitor survivin and HLA class I. In pattern B, 100% of all islets contained normal-appearing but quantitatively reduced beta cells without survivin or HLA class I. Conclusions/interpretation Our data demonstrate that C-peptide secretion in long-standing diabetic patients can be explained by two different patterns of beta cell survival, possibly reflecting different subsets of type 1 diabetes.
AbstractList	Aims/hypothesis Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells. Analysis of C-peptide in children characterised at diabetes onset for autoantibodies shows heterogeneous preservation of insulin secretion in long-standing diabetes. The aim of this study was to characterise the pancreases of childhood-onset diabetes in order to define the pathological basis of this heterogeneity. Methods We evaluated 20 cadaveric organ donor pancreases of childhood-onset long-term patients for disease heterogeneity and obtained corresponding C-peptide measurements. Results Pancreases from the majority of cadaveric donors contained only insulin-deficient islets (14 of 20). The remaining six patients (30%) had numerous insulin-positive cells within at least some islets, with two different histological patterns. Pattern A (which we would associate with type 1A diabetes) had lobular retention of areas with ‘abnormal' beta cells producing the apoptosis inhibitor survivin and HLA class I. In pattern B, 100% of all islets contained normal-appearing but quantitatively reduced beta cells without survivin or HLA class I. Conclusions/interpretation Our data demonstrate that C-peptide secretion in long-standing diabetic patients can be explained by two different patterns of beta cell survival, possibly reflecting different subsets of type 1 diabetes. Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells. Analysis of C-peptide in children characterised at diabetes onset for autoantibodies shows heterogeneous preservation of insulin secretion in long-standing diabetes. The aim of this study was to characterise the pancreases of childhood-onset diabetes in order to define the pathological basis of this heterogeneity. We evaluated 20 cadaveric organ donor pancreases of childhood-onset long-term patients for disease heterogeneity and obtained corresponding C-peptide measurements. Pancreases from the majority of cadaveric donors contained only insulin-deficient islets (14 of 20). The remaining six patients (30%) had numerous insulin-positive cells within at least some islets, with two different histological patterns. Pattern A (which we would associate with type 1A diabetes) had lobular retention of areas with 'abnormal' beta cells producing the apoptosis inhibitor survivin and HLA class I. In pattern B, 100% of all islets contained normal-appearing but quantitatively reduced beta cells without survivin or HLA class I. Our data demonstrate that C-peptide secretion in long-standing diabetic patients can be explained by two different patterns of beta cell survival,possibly reflecting different subsets of type 1 diabetes. Aims/hypothesis Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells. Analysis of C-peptide in children characterised at diabetes onset for autoantibodies shows heterogeneous preservation of insulin secretion in long-standing diabetes. The aim of this study was to characterise the pancreases of childhood-onset diabetes in order to define the pathological basis of this heterogeneity. Methods We evaluated 20 cadaveric organ donor pancreases of childhood-onset long-term patients for disease heterogeneity and obtained corresponding C-peptide measurements. Results Pancreases from the majority of cadaveric donors contained only insulin-deficient islets (14 of 20). The remaining six patients (30%) had numerous insulin-positive cells within at least some islets, with two different histological patterns. Pattern A (which we would associate with type 1A diabetes) had lobular retention of areas with ‘abnormal’ beta cells producing the apoptosis inhibitor survivin and HLA class I. In pattern B, 100% of all islets contained normal-appearing but quantitatively reduced beta cells without survivin or HLA class I. Conclusions/interpretation Our data demonstrate that C-peptide secretion in long-standing diabetic patients can be explained by two different patterns of beta cell survival, possibly reflecting different subsets of type 1 diabetes. Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells. Analysis of C-peptide in children characterised at diabetes onset for autoantibodies shows heterogeneous preservation of insulin secretion in long-standing diabetes. The aim of this study was to characterise the pancreases of childhood-onset diabetes in order to define the pathological basis of this heterogeneity. We evaluated 20 cadaveric organ donor pancreases of childhood-onset long-term patients for disease heterogeneity and obtained corresponding C-peptide measurements. Pancreases from the majority of cadaveric donors contained only insulin-deficient islets (14 of 20). The remaining six patients (30%) had numerous insulin-positive cells within at least some islets, with two different histological patterns. Pattern A (which we would associate with type 1A diabetes) had lobular retention of areas with 'abnormal' beta cells producing the apoptosis inhibitor survivin and HLA class I. In pattern B, 100% of all islets contained normal-appearing but quantitatively reduced beta cells without survivin or HLA class I. Our data demonstrate that C-peptide secretion in long-standing diabetic patients can be explained by two different patterns of beta cell survival, possibly reflecting different subsets of type 1 diabetes.[PUBLICATION ABSTRACT] Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells. Analysis of C-peptide in children characterised at diabetes onset for autoantibodies shows heterogeneous preservation of insulin secretion in long-standing diabetes. The aim of this study was to characterise the pancreases of childhood-onset diabetes in order to define the pathological basis of this heterogeneity.AIMS/HYPOTHESISChildhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells. Analysis of C-peptide in children characterised at diabetes onset for autoantibodies shows heterogeneous preservation of insulin secretion in long-standing diabetes. The aim of this study was to characterise the pancreases of childhood-onset diabetes in order to define the pathological basis of this heterogeneity.We evaluated 20 cadaveric organ donor pancreases of childhood-onset long-term patients for disease heterogeneity and obtained corresponding C-peptide measurements.METHODSWe evaluated 20 cadaveric organ donor pancreases of childhood-onset long-term patients for disease heterogeneity and obtained corresponding C-peptide measurements.Pancreases from the majority of cadaveric donors contained only insulin-deficient islets (14 of 20). The remaining six patients (30%) had numerous insulin-positive cells within at least some islets, with two different histological patterns. Pattern A (which we would associate with type 1A diabetes) had lobular retention of areas with 'abnormal' beta cells producing the apoptosis inhibitor survivin and HLA class I. In pattern B, 100% of all islets contained normal-appearing but quantitatively reduced beta cells without survivin or HLA class I.RESULTSPancreases from the majority of cadaveric donors contained only insulin-deficient islets (14 of 20). The remaining six patients (30%) had numerous insulin-positive cells within at least some islets, with two different histological patterns. Pattern A (which we would associate with type 1A diabetes) had lobular retention of areas with 'abnormal' beta cells producing the apoptosis inhibitor survivin and HLA class I. In pattern B, 100% of all islets contained normal-appearing but quantitatively reduced beta cells without survivin or HLA class I.Our data demonstrate that C-peptide secretion in long-standing diabetic patients can be explained by two different patterns of beta cell survival,possibly reflecting different subsets of type 1 diabetes.CONCLUSIONS/INTERPRETATIONOur data demonstrate that C-peptide secretion in long-standing diabetic patients can be explained by two different patterns of beta cell survival,possibly reflecting different subsets of type 1 diabetes.
Author	Solis, J. M Wasserfall, C Gianani, R West, E Kent, S. C Bonner-Weir, S Hering, B. J Eisenbarth, G. S Coppieters, K Sarkar, S. A Pugliese, A von Herrath, M Steck, A Campbell-Thompson, M Atkinson, M. A
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Keywords	Islet autoantibodies Childhood diabetes Type 1 diabetes HLA DR3 HLA DR4 Autoimmune diabetes Patterns of beta cell loss Pathology of childhood diabetes Heterogeneity of diabetes Organ donors Endocrinopathy Autoimmunity Immunopathology HLA-System Langerhans islet Autoantibody Autoimmune disease Anatomic pathology Histopathology Donor β Cell Endocrine pancreas
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PublicationDate_xml	– month: 04 year: 2010 text: 2010-04-01 day: 01
PublicationDecade	2010
PublicationPlace	Berlin/Heidelberg
PublicationPlace_xml	– name: Berlin/Heidelberg – name: Heidelberg – name: Germany
PublicationSubtitle	Clinical and Experimental Diabetes and Metabolism
PublicationTitle	Diabetologia
PublicationTitleAbbrev	Diabetologia
PublicationTitleAlternate	Diabetologia
PublicationYear	2010
Publisher	Berlin/Heidelberg : Springer-Verlag Springer-Verlag Springer Springer Nature B.V
Publisher_xml	– name: Berlin/Heidelberg : Springer-Verlag – name: Springer-Verlag – name: Springer – name: Springer Nature B.V
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mellitus: a predictable autoimmune disease with interindividual variation in the rate of beta cell destruction publication-title: Clin Immunol Immunopathol doi: 10.1016/0090-1229(89)90115-3 – volume: 85 start-page: 1263 year: 2005 end-page: 1275 ident: CR13 article-title: Parenchymal regression in chronic pancreatitis spares islets reprogrammed for the expression of NF kappa B and IAPs publication-title: Lab Invest doi: 10.1038/labinvest.3700323 – volume: 58 start-page: A459 issue: Suppl 1 year: 2009 ident: CR8 article-title: C-peptide levels correlate with age of onset, duration of diabetes and autoantibody status publication-title: Diabetes – volume: 4 start-page: 469 year: 2003 end-page: 477 ident: CR16 article-title: Insulin resistance and risk of chronic kidney disease in nondiabetic US adults publication-title: J Am Soc Nephrol doi: 10.1097/01.ASN.0000046029.53933.09 – volume: 155 start-page: 125 year: 2009 end-page: 127 ident: CR1 article-title: Post-mortem analysis of islet pathology in type 1 diabetes illuminates the life and death of the beta cell publication-title: Clin Exp Immunol doi: 10.1111/j.1365-2249.2008.03864.x – volume: 88 start-page: 5090 year: 2003 end-page: 5098 ident: CR5 article-title: Ketosis-prone diabetes: dissection of a heterogeneous syndrome using an immunogenetic and beta-cell functional classsification, prospective analysis, and clinical outcomes publication-title: J Clin Endocrinol Metab doi: 10.1210/jc.2003-030180 – volume: 30 start-page: 757 year: 2004 end-page: 762 ident: CR10 article-title: Residual insulin positivity and pancreatic atrophy in relation to duration of chronic type 1 (insulin-dependent) diabetes mellitus and microangiopathy publication-title: Diabetologia – volume: 14 start-page: 619 year: 1965 end-page: 633 ident: CR11 article-title: Pathologic anatomy of the pancreas in juvenile diabetes mellitus publication-title: Diabetes – volume: 292 start-page: 2 year: 2008 end-page: 13 ident: CR17 article-title: Pancreatic pathology in type 1 diabetes in humans publication-title: Novartis Found Symp doi: 10.1002/9780470697405.ch2 – volume: 344 start-page: 1588 year: 2008 end-page: 1592 ident: CR6 article-title: Neonatal diabetes mellitus due to complete glucokinase deficiency publication-title: N Engl J Med doi: 10.1056/NEJM200105243442104 – volume: 6 start-page: 392 year: 2008 ident: 1642_CR12 publication-title: Pediatr Dev Pathol doi: 10.1007/s10024-003-2014-0 – volume: 58 start-page: A459 issue: Suppl 1 year: 2009 ident: 1642_CR8 publication-title: Diabetes – volume: 57 start-page: 2718 year: 2008 ident: 1642_CR14 publication-title: Diabetes doi: 10.2337/db08-0170 – volume: 4 start-page: 469 year: 2003 ident: 1642_CR16 publication-title: J Am Soc Nephrol doi: 10.1097/01.ASN.0000046029.53933.09 – volume: 204 start-page: 232 year: 2005 ident: 1642_CR3 publication-title: Immunol Rev doi: 10.1111/j.0105-2896.2005.00248.x – volume: 88 start-page: 5090 year: 2003 ident: 1642_CR5 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Snippet	Aims/hypothesis Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells.... Aims/hypothesis Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells.... Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells. Analysis of C-peptide...
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SubjectTerms	Adolescent Adult African Americans Age of Onset Apoptosis Autoantibodies Autoantibodies - blood Autoimmune diabetes Autopsies Biological and medical sciences blood C-Peptide C-Peptide - blood Child Child, Preschool Childhood diabetes Diabetes Diabetes Mellitus, Type 1 Diabetes Mellitus, Type 1 - immunology Diabetes Mellitus, Type 1 - pathology Diabetes. Impaired glucose tolerance Endocrine pancreas. Apud cells (diseases) Endocrinopathies Etiopathogenesis. Screening. Investigations. Target tissue resistance Female Heterogeneity of diabetes Hispanic people Histocompatibility Testing Histopathology HLA DR3 HLA DR4 HLA-DR Antigens Human Physiology Humans Hyperinsulinism Hyperinsulinism - pathology immunology Insulin insulin-dependent diabetes mellitus Insulin-Secreting Cells Insulin-Secreting Cells - pathology Internal Medicine Islet autoantibodies Male Medical sciences Medicine Medicine & Public Health Metabolic Diseases Middle Aged Organ donors Pancreas Pancreas - pathology Pathology Pathology of childhood diabetes Patterns of beta cell loss Peptides Sex Characteristics Tissue Donors
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Title	Dimorphic histopathology of long-standing childhood-onset diabetes
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