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首页> 外文期刊>Structure >Structure and Sequence Analyses of Clustered Protocadherins Reveal Antiparallel Interactions that Mediate Homophilic Specificity
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Structure and Sequence Analyses of Clustered Protocadherins Reveal Antiparallel Interactions that Mediate Homophilic Specificity

机译:簇原钙粘蛋白的结构和序列分析揭示介导亲和力特异性的反平行相互作用。

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摘要

Clustered protocadherin (Pcdh) proteins mediate dendritic self-avoidance in neurons via specific homophilic interactions in their extracellular cadherin (EC) domains. We determined crystal structures of EC1-EC3, containing the homophilic specificity-determining region, of two mouse clustered Pcdh isoforms (Pcdh gamma A1 and Pcdh gamma C3) to investigate the nature of the homophilic interaction. Within the crystal lattices, we observe antiparallel interfaces consistent with a role in trans cell-cell contact. Antiparallel dimerization is supported by evolutionary correlations. Two interfaces, located primarily on EC2-EC3, involve distinctive clustered Pcdh structure and sequence motifs, lack predicted glycosylation sites, and contain residues highly conserved in orthologs but not paralogs, pointing toward their biological significance as homophilic interaction interfaces. These two interfaces are similar yet distinct, reflecting a possible difference in interaction architecture between clustered Pcdh subfamilies. These structures initiate a molecular understanding of clustered Pcdh assemblies that are required to produce functional neuronal networks.
机译:簇状原钙黏着蛋白(Pcdh)蛋白通过其细胞外钙黏着蛋白(EC)域中的特定同源相互作用介导神经元中的树突状自我回避。我们确定EC1-EC3的晶体结构,其中包含两个小鼠聚簇的Pcdh亚型(Pcdh gamma A1和Pcdh gamma C3)的同源性确定区域,以研究同源性相互作用的性质。在晶格内,我们观察到反平行界面与跨细胞-细胞接触中的作用一致。进化相关性支持反平行二聚化。主要位于EC2-EC3上的两个界面均具有独特的簇状Pcdh结构和序列基序,缺乏预测的糖基化位点,并且含有在直系同源物中高度保守的残基,而在旁系同源物中则高度保守,这表明它们的生物学意义是同源相互作用的界面。这两个接口相似但又截然不同,反映出群集的Pcdh子家族之间的交互体系结构可能存在差异。这些结构启动了对产生功能性神经元网络所需的簇状Pcdh组件的分子理解。

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