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Ku自身抗原70-kDa亚基的抗原决定簇

Antigenic determinants of the 70-kDa subunit of the Ku autoantigen.

作者信息

Abu-Elheiga L, Yaneva M

机构信息

Department of Pharmacology, Baylor College of Medicine Houston, Texas 77030.

出版信息

Clin Immunol Immunopathol. 1992 Aug;64(2):145-52. doi: 10.1016/0090-1229(92)90192-q.

Abstract

Autoantibodies against Ku antigen were found in subsets of sera from patients with rheumatic diseases. The Ku autoantigen was characterized as a DNA-binding protein complex composed of two subunits, 70 and 86 kDa. In this study, we report the amino acid sequences of the 70-kDa subunit that are important for interactions with a monoclonal and autoimmune antibodies. Full-length cDNA and numerous 5' and 3' deletion mutants were expressed in bacteria and the immunoreactivity of the fusion proteins was analyzed by Western blotting. The reactivity of the monoclonal antibody depended on the region between Ile321 and Phe350. Ten autoimmune sera were tested for reactivity with deletion mutants in immunoblots. The reactivity of six sera strongly depended on the C-terminal amino acids and four sera did not show such dependence; however, these C-terminal sequences did not react with the sera when expressed alone. These results strongly suggest the conformational nature of the Ku autoepitopes. Interestingly, the DNA-binding activity of this Ku protein subunit analyzed by Southwestern blot depended on the same C-terminal amino acids that were involved in interactions with autoantibodies, indicating that anti-Ku autoantibodies are directed to conformationally intact Ku antigen. Reactivities of the autoimmune sera with Met1-Arg115, Met116-Val149, and Val149-Arg586 were also observed. These results demonstrate that different amino acid regions can be involved in interactions with autoimmune antibodies.

摘要

在风湿性疾病患者的部分血清中发现了针对Ku抗原的自身抗体。Ku自身抗原被鉴定为一种由两个亚基(70 kDa和86 kDa)组成的DNA结合蛋白复合物。在本研究中,我们报告了70 kDa亚基与单克隆抗体和自身免疫抗体相互作用的重要氨基酸序列。全长cDNA以及众多5'和3'缺失突变体在细菌中表达,并通过蛋白质免疫印迹分析融合蛋白的免疫反应性。单克隆抗体的反应性取决于Ile321和Phe350之间的区域。在免疫印迹中测试了10份自身免疫血清与缺失突变体的反应性。6份血清的反应性强烈依赖于C末端氨基酸,4份血清则没有这种依赖性;然而,这些C末端序列单独表达时不与血清反应。这些结果强烈表明Ku自身表位的构象性质。有趣的是,通过蛋白质免疫印迹分析的该Ku蛋白亚基的DNA结合活性取决于与自身抗体相互作用所涉及的相同C末端氨基酸,这表明抗Ku自身抗体针对的是构象完整的Ku抗原。还观察到自身免疫血清与Met1-Arg115、Met116-Val149和Val149-Arg586的反应性。这些结果表明不同的氨基酸区域可参与与自身免疫抗体的相互作用。

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