ISLET-REACTIVE T-CELLS ARE A MARKER OF PRECLINICAL INSULIN-DEPENDENT DIABETES

Harrison, LC; CHU, SX; DeAizpurua, HJ; GRAHAM, M; Honeyman, MC; Colman, PG

Author(s): Harrison, LC; CHU, SX; DeAizpurua, HJ; GRAHAM, M; Honeyman, MC; Colman, PG;
Details: Publication Year 1992-04,Volume 89,Issue #4,Page 1161-1165
Journal Title: JOURNAL OF CLINICAL INVESTIGATION
Publication Type: Journal Article
Abstract: The destruction of pancreatic islet beta cells in insulin-dependent diabetes mellitus (IDDM) is thought to be T cell mediated. To directly identify islet-reactive T cells in asymptomatic, "preclinical" IDDM individuals with islet cell antibodies (ICA), proliferation of peripheral blood mononuclear cells (PBMC) was measured in the presence of sonicated fetal pig proislets. Stimulation indices (mean +/- SD) for [H-3]thymidine uptake by PBMC cultured with sonicated proislets were: preclinical IDDM subjects (n = 22) 6.10 +/- 6.50, recent-onset IDDM subjects (n = 29) 3.66 +/- 3.35, Graves' disease subjects (n = 6) 2.17 +/- 0.93, scleroderma subjects (n = 4) 1.65 +/- 0.19 and normal control subjects (n = 14) 1.63 +/- 0.62. 68% (15/22) of preclinical IDDM, 41% (12/29) of recent-onset IDDM and 17% (1/6) of Graves' disease subjects had T cell reactivity greater than the mean + 2 SD of controls. T cell reactivity to proislets with tissue specific, and greater in magnitude and frequency than to human insulin. The majority of preclinical subjects with ICA > 20 Juvenile Diabetes Foundation (JDF) units (12/15, 80%) or antibodies to a 64-kD islet autoantigen (11/15, 73%) had significant T cell reactivity to proislets. ICA > 40 JDF units, a strong prognostic marker for progression to clinical IDDM, was an absolute index of T cell reactivity. Overall, the frequency of T cell reactivity in preclinical subjects, 68% (15/22), was comparable to that of ICA > 20 JDF units or 64-kD antibodies. Greater T cell reactivity to proislets in preclinical subjects accords with the natural history of autoimmune beta cell destruction. The direct assay of islet-reactive T cells in peripheral blood may have prognostic significance for the development of clinical IDDM and should facilitate identification of the primary target autoantigen(s).
Publisher: ROCKEFELLER UNIV PRESS
Keywords: MELLITUS; MICE; RAT
Publisher's Version: https://doi.org/10.1172/JCI115698
Terms of Use/Rights Notice: Refer to copyright notice on published article.

Creation Date: 1992-04-01 12:00:00