Etiopathogenesis of insulin autoimmunity.

Anatomy research international Pub Date : 2012-01-01 Epub Date: 2012-02-22 DOI:10.1155/2012/457546
Norio Kanatsuna, George K Papadopoulos, Antonis K Moustakas, Ake Lenmark
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Abstract

Autoimmunity against pancreatic islet beta cells is strongly associated with proinsulin, insulin, or both. The insulin autoreactivity is particularly pronounced in children with young age at onset of type 1 diabetes. Possible mechanisms for (pro)insulin autoimmunity may involve beta-cell destruction resulting in proinsulin peptide presentation on HLA-DR-DQ Class II molecules in pancreatic draining lymphnodes. Recent data on proinsulin peptide binding to type 1 diabetes-associated HLA-DQ2 and -DQ8 is reviewed and illustrated by molecular modeling. The importance of the cellular immune reaction involving cytotoxic CD8-positive T cells to kill beta cells through Class I MHC is discussed along with speculations of the possible role of B lymphocytes in presenting the proinsulin autoantigen over and over again through insulin-carrying insulin autoantibodies. In contrast to autoantibodies against other islet autoantigens such as GAD65, IA-2, and ZnT8 transporters, it has not been possible yet to standardize the insulin autoantibody test. As islet autoantibodies predict type 1 diabetes, it is imperative to clarify the mechanisms of insulin autoimmunity.

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胰岛素自身免疫的发病机制。
针对胰岛β细胞的自身免疫与胰岛素原、胰岛素或两者都有密切关系。胰岛素自身反应性在 1 型糖尿病发病年龄较小的儿童中尤为明显。促)胰岛素自身免疫的可能机制可能是β细胞破坏导致胰腺引流淋巴结中的 HLA-DR-DQ II 类分子上出现促胰岛素肽。本文回顾了胰岛素原肽与 1 型糖尿病相关 HLA-DQ2 和 -DQ8 结合的最新数据,并通过分子建模进行了说明。文章讨论了细胞毒性 CD8 阳性 T 细胞通过 I 类 MHC 杀死 beta 细胞的细胞免疫反应的重要性,并推测了 B 淋巴细胞在通过携带胰岛素的胰岛素自身抗体反复呈现胰岛素原自身抗原方面可能扮演的角色。与针对其他胰岛自身抗原(如 GAD65、IA-2 和 ZnT8 转运体)的自身抗体不同,胰岛素自身抗体检测尚未实现标准化。由于胰岛自身抗体可预测 1 型糖尿病,因此必须明确胰岛素自身免疫的机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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