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Diabetes, Vol 45, Issue 10 1299-1305, Copyright © 1996 by American Diabetes Association
Diabetogenic T-cell clones
K Haskins and D Wegmann
Barbara Davis Center for Childhood Diabetes, Department of Immunology, University of Colorado Health Sciences Center, Denver 80262, USA.
The role of T-cells in the pathogenesis of IDDM has been an area of much
interest, and investigators have recently acquired new tools for studies on
T-cells with the advent of T-cell clones that are reactive with islet
antigens. Derived from NOD mice, diabetogenic T-cell lines and clones have
for the most part been CD4+ and T-helper 1 (Th1)-like in their cytokine
production. Some CD8+ cytotoxic clones have also been reported, although
these have generally not transferred diabetes in the absence of CD4+
T-cells. The T-cell clones that have been described can also be separated
on the basis of their antigen reactivity. While many of the T-cell lines
and clones described react with islets, isolated islet cells, or islet
membrane preparations, others have known antigen specificities, reacting
with defined islet cell proteins such as insulin, GAD, and heat shock
proteins. Particularly in the case of insulin-reactive clones,
diabetogenicity has also been demonstrated. In light of the many possible
T-cell reactivities that may arise from the islet lesion, the question of
whether there is a dominant initiating antigen is a particularly intriguing
one.

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Copyright © 1996 by the American Diabetes Association.
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