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从一名1型糖尿病患者体内分离出的四种抗胰岛人源单克隆IgG抗体识别谷氨酸脱羧酶65的不同表位,且存在体细胞突变。

Four IgG anti-islet human monoclonal antibodies isolated from a type 1 diabetes patient recognize distinct epitopes of glutamic acid decarboxylase 65 and are somatically mutated.

作者信息

Madec A M, Rousset F, Ho S, Robert F, Thivolet C, Orgiazzi J, Lebecque S

机构信息

INSERM Unit 449, R. Laennec Faculty of Medicine, Lyon, France.

出版信息

J Immunol. 1996 May 1;156(9):3541-9.

PMID:8617984
Abstract

The selective destruction by an autoimmune process of the beta cells in the pancreas is the hallmark of the type 1 insulin-dependent diabetes mellitus. What triggers islet cell-specific autoreactive T and B cells, however, remains unclear. Identification of the targets of the anti-islet cell autoantibodies frequently found in insulin-dependent diabetes mellitus patients and analysis of their sequences should provide some insights into the nature of this disease. We have combined EBV transformation with CD40 activation of peripheral B cells from one patient with insulin-dependent diabetes mellitus to isolate four B cell clones that secrete islet cell-specific autoantibodies, These four human monoclonal autoantibodies are of the IgG1 isotype, and they each recognize a different epitope of the glutamic acid decarboxylase enzyme. Analysis of their variable gene sequences shows that, while clonally unrelated, three of the four human monoclonal autoantibodies use a member of the VH4 family, and two have rearranged the same delta light chain variable gene. The IgG1 isotype of the four autoantibodies as well as the presence of somatic mutations in both heavy and light chain genes provide concrete evidence for their derivation by a T cell-dependent immune response.

摘要

胰腺中β细胞因自身免疫过程而被选择性破坏是1型胰岛素依赖型糖尿病的标志。然而,引发胰岛细胞特异性自身反应性T细胞和B细胞的因素仍不清楚。鉴定胰岛素依赖型糖尿病患者中常见的抗胰岛细胞自身抗体的靶标并分析其序列,应能为这种疾病的本质提供一些见解。我们将EBV转化与来自一名胰岛素依赖型糖尿病患者的外周血B细胞的CD40激活相结合,分离出四个分泌胰岛细胞特异性自身抗体的B细胞克隆。这四种人源单克隆自身抗体属于IgG1同种型,它们各自识别谷氨酸脱羧酶的不同表位。对其可变基因序列的分析表明,虽然这四个克隆不相关,但其中三种人源单克隆自身抗体使用VH4家族的一个成员,并且有两种重排了相同的δ轻链可变基因。这四种自身抗体的IgG1同种型以及重链和轻链基因中体细胞突变的存在,为它们通过T细胞依赖性免疫反应产生提供了确凿证据。

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