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Diabetes Care, Vol 20, Issue 4 524-529, Copyright © 1997 by American Diabetes Association
Distinct genetic and immunological features in patients with onset of IDDM before and after age 40
T Lohmann, J Sessler, HJ Verlohren, S Schroder, J Rotger, K Dahn, N Morgenthaler and WA Scherbaum
Department of Internal Medicine III, University of Leipzig, Germany.
OBJECTIVE: Young age at onset is a relevant parameter associated with a
rapid progression of IDDM. Our major aim was to define differences between
IDDM patients with age at diagnosis > 40 years and adult IDDM with onset
at a younger age. RESEARCH DESIGN AND METHODS: The correlation between
islet-related antibodies (islet cell antibodies [ICAs] and antibodies [Abs]
to GAD and the tyrosine phosphatase IA2), T-cell responses to GAD peptides
and HLA class II isotypes was investigated in 23 IDDM patients 12-38 years
of age at onset (group 1), 24 patients with IDDM > 40 years of age at
onset (group 2), and 12 healthy control subjects. ICAs were measured by
indirect immunofluorescence, and GAD-Ab and IA2-Ab were measured by
immunoprecipitation tests. T-cell responses against GAD peptides, which had
been identified as typical for IDDM, were tested by 5-day proliferation
assays. HLA class II alleles were typed by polymerase chain reaction.
RESULTS: ICAs and GAD-Abs were more prevalent in IDDM patients than in
control subjects (P < 0.001), but only IDDM group 1 had IA2-Abs (P <
0.001 compared with IDDM group 2 and control subjects). Moreover, antibody
combinations differed between IDDM patients of groups 1 and 2. T-cell
responses to GAD peptides were seen in 67% of IDDM group 1 and in 71% of
IDDM group 2 (P < 0.02 compared with control subjects). IDDM patients of
group 1 were more frequently DR4+/DQ8+ and less frequently DR2+/DQ0602+
compared with IDDM patients of group 2 (P < 0.05). CONCLUSIONS: Our data
provide strong evidence for humoral and cellular autoimmunity in adult IDDM
patients with onset both before and after 40 years of age. However,
late-onset differs from young-onset IDDM with respect to Ab profiles,
especially a lack of IA2-Ab, and HLA class II types. These findings have
consequences for the diagnostic strategy for identifying slow-onset IDDM in
individuals after 40 years of age.

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Copyright © 1997 by the American Diabetes Association.
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