Glutamate decarboxylase (GAD) autoantibody epitope shift during the first year of Type 1 diabetes

Hampe, C. S.; Örtqvist, E.; Persson, B.; Schranz, D. B.; Lernmark, Å

Glutamate decarboxylase (GAD) autoantibody epitope shift during the first year of Type 1 diabetes

Mark

Hampe, C. S. ; Örtqvist, E. ; Persson, B. ; Schranz, D. B. and Lernmark, Å ^LU

(1999) In Hormone and Metabolic Research 31(10). p.553-557

Abstract: Autoantibodies in Type 1 diabetes patients may differentiate between glutamate decarboxylase (GAD65) cloned from human, mouse and rat with a significant better binding to the human antigen. A subgroup of 15% (27/183) patients showed significantly better binding to rodent than to human GAD65. The aim of this study was to determine whether the autoantibody specificity would remain anti-rodent during longitudinal follow-up for one year. We observed 1) that the average slope of the difference between human and mouse GAD65 autoantibodies binding increased between onset and after one year, which demonstrates reduced binding to rodent GAD65 and 2) that, in a group followed every third month, 9/11 (80%) children with rodent specific GAD65... (More); Autoantibodies in Type 1 diabetes patients may differentiate between glutamate decarboxylase (GAD65) cloned from human, mouse and rat with a significant better binding to the human antigen. A subgroup of 15% (27/183) patients showed significantly better binding to rodent than to human GAD65. The aim of this study was to determine whether the autoantibody specificity would remain anti-rodent during longitudinal follow-up for one year. We observed 1) that the average slope of the difference between human and mouse GAD65 autoantibodies binding increased between onset and after one year, which demonstrates reduced binding to rodent GAD65 and 2) that, in a group followed every third month, 9/11 (80%) children with rodent specific GAD65 autoantibodies at onset converted within one year to preference against human GAD65. This shift in preference was confirmed by significantly lower EC₅₀ values in the initially anti-rodent GAD65 autoantibodies compared to samples taken one year after clinical diagnosis as determined in displacement studies with unlabeled human GAD65. We speculate that the evolution of GAD65 autoantibodies in Type 1 diabetes includes reactivity to a non-human GAD65 N- terminal end conformation. Progression towards Type 1 diabetes is, however, associated with a maturation of the immune response towards human GAD65 autoreactivity.
(Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/375b1a5c-9cad-451d-894f-2ae7b91582a4

author

Hampe, C. S. ; Örtqvist, E. ; Persson, B. ; Schranz, D. B. and Lernmark, Å ^LU

publishing date

1999-01-01

type

Contribution to journal

publication status

published

subject

Endocrinology and Diabetes

keywords

Antibodies, Autoimmunity, Epitope Spreading

in

Hormone and Metabolic Research

volume

31

issue

10

pages

553 - 557

publisher

Georg Thieme Verlag

external identifiers

scopus:0032747140
pmid:10596964

ISSN

0018-5043

DOI

10.1055/s-2007-978794

language

English

LU publication?

no

id

375b1a5c-9cad-451d-894f-2ae7b91582a4

date added to LUP

2019-06-30 23:37:02

date last changed

2024-03-13 08:29:32

@article{375b1a5c-9cad-451d-894f-2ae7b91582a4,
  abstract     = {{<p>Autoantibodies in Type 1 diabetes patients may differentiate between glutamate decarboxylase (GAD65) cloned from human, mouse and rat with a significant better binding to the human antigen. A subgroup of 15% (27/183) patients showed significantly better binding to rodent than to human GAD65. The aim of this study was to determine whether the autoantibody specificity would remain anti-rodent during longitudinal follow-up for one year. We observed 1) that the average slope of the difference between human and mouse GAD65 autoantibodies binding increased between onset and after one year, which demonstrates reduced binding to rodent GAD65 and 2) that, in a group followed every third month, 9/11 (80%) children with rodent specific GAD65 autoantibodies at onset converted within one year to preference against human GAD65. This shift in preference was confirmed by significantly lower EC<sub>50</sub> values in the initially anti-rodent GAD65 autoantibodies compared to samples taken one year after clinical diagnosis as determined in displacement studies with unlabeled human GAD65. We speculate that the evolution of GAD65 autoantibodies in Type 1 diabetes includes reactivity to a non-human GAD65 N- terminal end conformation. Progression towards Type 1 diabetes is, however, associated with a maturation of the immune response towards human GAD65 autoreactivity.</p>}},
  author       = {{Hampe, C. S. and Örtqvist, E. and Persson, B. and Schranz, D. B. and Lernmark, Å}},
  issn         = {{0018-5043}},
  keywords     = {{Antibodies; Autoimmunity; Epitope Spreading}},
  language     = {{eng}},
  month        = {{01}},
  number       = {{10}},
  pages        = {{553--557}},
  publisher    = {{Georg Thieme Verlag}},
  series       = {{Hormone and Metabolic Research}},
  title        = {{Glutamate decarboxylase (GAD) autoantibody epitope shift during the first year of Type 1 diabetes}},
  url          = {{http://dx.doi.org/10.1055/s-2007-978794}},
  doi          = {{10.1055/s-2007-978794}},
  volume       = {{31}},
  year         = {{1999}},
}

Lund University Publications

LUND UNIVERSITY LIBRARIES

Glutamate decarboxylase (GAD) autoantibody epitope shift during the first year of Type 1 diabetes