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用单克隆抗体绘制人胰岛素受体的表面结构:主要免疫原性区域定位于受体激酶结构域。

Mapping surface structures of the human insulin receptor with monoclonal antibodies: localization of main immunogenic regions to the receptor kinase domain.

作者信息

Morgan D O, Roth R A

出版信息

Biochemistry. 1986 Mar 25;25(6):1364-71. doi: 10.1021/bi00354a026.

Abstract

A panel of 37 monoclonal antibodies to the human insulin receptor has been used to characterize the receptor's major antigenic regions and their relationship to receptor functions. Three antibodies recognized extracellular surface structures, including the insulin binding site and a region not associated with insulin binding. The remaining 34 monoclonal antibodies were directed against the cytoplasmic domain of the receptor beta subunit. Competitive binding studies demonstrated that four antigenic regions (beta 1, beta 2, beta 3, and beta 4) are found on this domain. Sixteen of the antibodies were found to be directed against beta 1, nine against beta 2, seven against beta 3, and two against beta 4. Antibodies to all four regions inhibited the receptor-associated protein kinase activity to some extent, although antibodies directed against the beta 2 region completely inhibited the kinase activity of the receptor both in the autophosphorylation reaction and in the phosphorylation of an exogenous substrate, histone. Antibodies to the beta 2 region also did not recognize autophosphorylated receptor. In addition, antibodies to this same region recognized the receptor for insulin-like growth factor I (IGF-I) as well as the insulin receptor. In contrast, antibodies to other cytoplasmic regions did not recognize the IGF-I receptor as well as the insulin receptor. These results indicate that the major immunogenic regions of the insulin receptor are located on the cytoplasmic domain of the receptor beta subunit and are associated with the tyrosine-specific kinase activity of the receptor. In addition, these results suggest that a portion of the insulin receptor is highly homologous to that of the IGF-I receptor.

摘要

一组针对人胰岛素受体的37种单克隆抗体被用于表征该受体的主要抗原区域及其与受体功能的关系。三种抗体识别细胞外表面结构,包括胰岛素结合位点和一个与胰岛素结合无关的区域。其余34种单克隆抗体则针对受体β亚基的细胞质结构域。竞争性结合研究表明,在该结构域上发现了四个抗原区域(β1、β2、β3和β4)。发现其中16种抗体针对β1,9种针对β2,7种针对β3,2种针对β4。针对所有四个区域的抗体在一定程度上抑制了受体相关的蛋白激酶活性,尽管针对β2区域的抗体在自身磷酸化反应和对外源底物组蛋白的磷酸化反应中都完全抑制了受体的激酶活性。针对β2区域的抗体也不能识别自身磷酸化的受体。此外,针对同一区域的抗体还能识别胰岛素样生长因子I(IGF-I)受体以及胰岛素受体。相比之下,针对其他细胞质区域的抗体不能像识别胰岛素受体那样识别IGF-I受体。这些结果表明,胰岛素受体的主要免疫原性区域位于受体β亚基的细胞质结构域上,并与受体的酪氨酸特异性激酶活性相关。此外,这些结果表明胰岛素受体的一部分与IGF-I受体高度同源。

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