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小鼠狼疮相关自身免疫反应的分子分析:大量重链和轻链可变区基因的参与

Molecular analysis of the murine lupus-associated anti-self response: involvement of a large number of heavy and light chain variable region genes.

作者信息

Kofler R, Noonan D J, Strohal R, Balderas R S, Møller N P, Dixon F J, Theofilopoulos A N

出版信息

Eur J Immunol. 1987 Jan;17(1):91-5. doi: 10.1002/eji.1830170116.

Abstract

The mRNA encoding heavy and light chains of a hybridoma-derived monoclonal IgM, kappa anti-immunoglobulin (rheumatoid factor) and an IgG3, kappa anti-histone autoantibody from systemic lupus erythematosus and arthritis-prone MRL/Mp-lpr/lpr mice have been molecularly cloned, and the nucleotide sequences corresponding to their variable regions have been determined. To investigate whether autoantibodies with specificities frequently observed in lupus disease might share common structural components, the sequences obtained in this study have been compared with those of a monoclonal MRL/Mp-lpr/lpr IgM, kappa anti-DNA autoantibody previously analyzed in our laboratory (J. Exp. Med. 1985. 161: 805). The 3 immunoglobulins employed different heavy chain variable region (VH) genes belonging to the large J588 VH gene family, kappa light chain variable region (V kappa) genes from 3 different V kappa groups, and different diversity and joining segments. Our findings suggest that murine lupus-associated autoantibodies of different specificities do not have genetic components in common to signal their self-reactive nature and are encoded by a large number of immunoglobulin gene elements.

摘要

已对源自杂交瘤的单克隆IgM、κ抗免疫球蛋白(类风湿因子)以及来自系统性红斑狼疮和易患关节炎的MRL/Mp-lpr/lpr小鼠的IgG3、κ抗组蛋白自身抗体的重链和轻链的mRNA进行了分子克隆,并确定了与其可变区相对应的核苷酸序列。为了研究在狼疮疾病中经常观察到的具有特异性的自身抗体是否可能共享共同的结构成分,已将本研究中获得的序列与先前在我们实验室分析的单克隆MRL/Mp-lpr/lpr IgM、κ抗DNA自身抗体的序列进行了比较(《实验医学杂志》1985年。161:805)。这3种免疫球蛋白使用了属于大J588 VH基因家族的不同重链可变区(VH)基因、来自3个不同Vκ组的κ轻链可变区(Vκ)基因以及不同的多样性和连接片段。我们的研究结果表明,不同特异性的小鼠狼疮相关自身抗体没有共同的遗传成分来表明它们的自身反应性本质,并且由大量免疫球蛋白基因元件编码。

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