INDUCTION AND THERAPY OF AUTOIMMUNE DIABETES IN THE NON-OBESE DIABETIC (NOD/LT) MOUSE BY A 65-KDA HEAT-SHOCK PROTEIN

被引：430

作者：

ELIAS, D

MARKOVITS, D

RESHEF, T

VANDERZEE, R

COHEN, IR

机构：

[1] WEIZMANN INST SCI,DEPT CELL BIOL,IL-76100 REHOVOT,ISRAEL

[2] NATL INST PUBL HLTH & ENVIRONM PROTECT,BILTHOVEN,NETHERLANDS

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1990年 / 87卷 / 04期

关键词：

Anti-idiotypic antibodies; Autoantibodies; T cells; Tolerance;

D O I：

10.1073/pnas.87.4.1576

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

Insulin-dependent diabetes mellitus is caused by autoimmune destruction of the insulin-producing beta cells of the pancreas. The results described here indicate that a beta-cell target antigen in non-obese diabetic (NOD/Lt) mice is a molecule cross-reactive with the 65-kDa heat shock protein (hsp65) of Mycobacterium tuberculosis. The onset of beta-cell destruction is associated with the spontaneous development of anti-hsp65 T lymphocytes. Subsequently hsp65 cross-reactive antigen becomes detectable in the sera of the prediabetic mice and some weeks later anti-hsp65 antibodies, anti-insulin antibodies, and anti-idiotypic antibodies to insulin antibodies become detectable. The hsp65-cross-reactive antigen, the auto-antibodies, and the T-cell reactivity then decline with the development of overt insulin-dependent diabetes. The importance of hsp65 in the pathogenesis of insulin-dependent diabetes was confirmed by the ability of clones of anti-hsp65 T cells to cause insulitis and hyperglycemia in young NOD/Lt mice. Moreover, hsp65 antigen could be used either to induce diabetes or to vaccinate against diabetes, depending on the form of its administration to prediabetic NOD/Lt mice. Other antigens such as the 70-kDa heat shock protein (hsp70) had no effect on the development of diabetes.

引用

页码：1576 / 1580

页数：5

共 19 条

[1] AUTOANTIBODIES IN NEWLY DIAGNOSED DIABETIC CHILDREN IMMUNOPRECIPITATE HUMAN PANCREATIC-ISLET CELL-PROTEINS
BAEKKESKOV, S
NIELSEN, JH
MARNER, B
BILDE, T
LUDVIGSSON, J
LERNMARK, A
[J]. NATURE, 1982, 298 (5870) : 167 - 169
[2] SYNGENEIC TRANSFER OF AUTOIMMUNE DIABETES FROM DIABETIC NOD MICE TO HEALTHY NEONATES - REQUIREMENT FOR BOTH L3T4+ AND LYT-2+ T-CELLS
BENDELAC, A
CARNAUD, C
BOITARD, C
BACH, JF
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1987, 166 (04) : 823 - 832
[3] A PILOT TRIAL OF COP-1 IN EXACERBATING REMITTING MULTIPLE-SCLEROSIS
BORNSTEIN, MB
MILLER, A
SLAGLE, S
WEITZMAN, M
CRYSTAL, H
DREXLER, E
KEILSON, M
MERRIAM, A
WASSERTHEILSMOLLER, S
SPADA, V
WEISS, W
ARNON, R
JACOBSOHN, I
TEITELBAUM, D
SELA, M
[J]. NEW ENGLAND JOURNAL OF MEDICINE, 1987, 317 (07) : 408 - 414
[4] THE SELF, THE WORLD AND AUTOIMMUNITY
COHEN, IR
[J]. SCIENTIFIC AMERICAN, 1988, 258 (04) : 52 - &
[5] DESENSITIZATION OF THE INSULIN-RECEPTOR BY ANTIRECEPTOR ANTIBODIES INVIVO IS BLOCKED BY TREATMENT OF MICE WITH BETA-ADRENERGIC AGONISTS
ELIAS, D
RAPOPORT, M
COHEN, IR
SHECHTER, Y
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1988, 81 (06) : 1979 - 1985
[6] ELIAS D, 1984, J BIOL CHEM, V259, P6416
[7] ARTHRITIS INDUCED IN RATS BY CLONED LYMPHOCYTES-T RESPONSIVE TO MYCOBACTERIA BUT NOT TO COLLAGEN TYPE-II
HOLOSHITZ, J
MATITIAU, A
COHEN, IR
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1984, 73 (01) : 211 - 215
[8] PRIMARY STRUCTURE OF A HUMAN MITOCHONDRIAL PROTEIN HOMOLOGOUS TO THE BACTERIAL AND PLANT CHAPERONINS AND TO THE 65-KILODALTON MYCOBACTERIAL ANTIGEN
JINDAL, S
DUDANI, AK
SINGH, B
HARLEY, CB
GUPTA, RS
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1989, 9 (05) : 2279 - 2283
[9] MAPPING OF T-CELL EPITOPES USING RECOMBINANT ANTIGENS AND SYNTHETIC PEPTIDES
LAMB, JR
IVANYI, J
REES, ADM
ROTHBARD, JB
HOWLAND, K
YOUNG, RA
YOUNG, DB
[J]. EMBO JOURNAL, 1987, 6 (05) : 1245 - 1249
[10] MARON R, 1983, J IMMUNOL, V131, P2316

← 1 2 →