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Topography of N-CAM structural and functional determinants. I. Classification of monoclonal antibody epitopes

机译:N-CAM结构和功能决定因素的形貌。一,单克隆抗体表位的分类

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摘要

12 distinct neural cell adhesion molecule (N-CAM) epitopes, each recognized by a different monoclonal antibody (mAb), have been characterized in terms of the major structural and functional features of the molecule. Seven antibodies, each recognizing the amino-terminal region of the molecule, altered the rate of N-CAM-mediated adhesion. Four of these were inhibitors, two of which also recognized a heparin- binding N-CAM fragment. The other three antibodies specifically enhanced the rate of N-CAM-mediated adhesion. Three epitopes, one polypeptide- and two carbohydrate-dependent, were associated with the sialic acid-rich central portion of the molecule. The remaining two antibodies were found to react with intracellular determinants, and are specific for the largest of the three major N-CAM polypeptide forms. Studies on the ability of one antibody to hinder recognition of native N-CAM by another antibody suggested that the epitopes associated with N- CAM binding functions are in close proximity compared with the other determinants. The classification of these mAb epitopes has allowed the topographical placement of key N-CAM features, as described in the following paper, and provides valuable probes for analysis of both the structure and function of N-CAM.
机译:根据该分子的主要结构和功能特征,已表征了12个不同的神经细胞粘附分子(N-CAM)表位,每个抗原表位均被不同的单克隆抗体(mAb)识别。七种抗体(各自识别分子的氨基末端区域)改变了N-CAM介导的粘附速率。这些中的四种是抑制剂,其中两种还识别结合肝素的N-CAM片段。其他三种抗体可特异性提高N-CAM介导的粘附率。三个表位,一种多肽依赖性和两种碳水化合物依赖性,与该分子富含唾液酸的中央部分相关。发现其余两种抗体与细胞内决定簇反应,并且对三种主要的N-CAM多肽形式中的最大形式具有特异性。对一种抗体阻碍另一种抗体识别天然N-CAM的能力的研究表明,与其他决定簇相比,与N-CAM结合功能相关的表位非常接近。这些mAb表位的分类已允许关键N-CAM特征的形貌定位,如下文所述,并为分析N-CAM的结构和功能提供了有价值的探针。

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  • 年度 1986
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  • 正文语种 {"code":"en","name":"English","id":9}
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