STUDIES ON AUTOIMMUNITY FOR INITIATION OF BETA-CELL DESTRUCTION .10. DELAYED EXPRESSION OF A MEMBRANE-BOUND ISLET CELL-SPECIFIC 38 KDA AUTOANTIGEN THAT PRECEDES INSULITIS AND DIABETES IN THE DIABETES-PRONE BB RAT

被引：13

作者：

KO, IY

JUN, HS

KIM, GS

YOON, JW

机构：

[1] UNIV CALGARY, FAC MED,JULIA MCFARLANE DIABET RES CTR, DEPT MICROBIOL & INFECT DIS,DIV VIROL, CALGARY T2N 4N1, AB, CANADA

[2] UNIV CALGARY, FAC MED,DEPT MICROBIOL & INFECT DIS,DIV VIROL, VIRAL & IMMUNOPATHOGENESIS DIABET LAB, CALGARY, AB, CANADA

来源：

DIABETOLOGIA | 1994年 / 37卷 / 05期

关键词：

ISLET CELL-SPECIFIC 38 KDA AUTOANTIGEN; IMMUNOLOGICAL EFFECTORS; BB RAT; AUTOIMMUNE IDDM;

D O I：

10.1007/s001250050132

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

The diabetic syndrome in the DP-BB rat results from progressive beta-cell destruction by autoimmune responses. However, the initial events causing the autoimmune destruction of beta cells remain largely unknown. Our recent experimental results suggest that the delayed expression of a beta-cell-specific autoantigen may result in the initiation of beta-cell-specific autoimmunity. The present investigation was initiated to identify such an autoantigen. Islets were isolated from DP-BB rats of several different ages, and protein extracts from the membrane fraction of the islet preparations were immunoprecipitated with sera from diabetic DP-BB rats. We have found that a membrane-bound islet cell-specific 38 kDa autoantigen is not expressed early in the life of DP-BB rats, but is delayed-expressed by approximately 30 days of age, the time at which immunological effecters begin to recognize beta cells. In contrast, a 64 kDa islet cell protein is expressed from birth in DP-BB rats. On the basis of these observations, we suggest that delayed expression of a gene encoding for the membrane-bound islet cell-specific 38 kDa autoantigen may result in a breakdown of self-tolerance, leading to beta-eel-specific autoimmune IDDM in the BB rat.

引用

页码：460 / 465

页数：6

共 22 条

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