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Single-Cell Identity Generated by Combinatorial Homophilic Interactions between α, β, and γ Protocadherins

机译:由α,β和γ原钙粘蛋白之间的组合亲和相互作用产生的单细胞身份

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摘要

Individual mammalian neurons stochastically express distinct repertoires of a, b, andγ protocadherin (Pcdh) proteins, which function in neural circuit assembly. We report that all three subfamilies of clustered Pcdhs can engage in specific homophilic interactions, that cell surface delivery of Pcdhα isoforms requires cis interactions with other Pcdhs, and that the extracellular cadherin domain EC6 plays a critical role in this process. Examination of homophilic interactions between specific combinations of multiple Pcdh isoforms revealed that Pcdh combinatorial recognition specificities depend on the identity of all of the expressed isoforms. A single mismatched Pcdh isoform can interfere with these combinatorial homophilic interactions. A theoretical analysis reveals that assembly of Pcdh isoforms into multimeric recognition units and the observed tolerance for mismatched isoforms can generate cell surface diversity sufficient for singlecell identity. However, the competing demands of nonself discrimination and self-recognition place limitations on the mechanisms by which homophilic recognition units can function.
机译:单个哺乳动物神经元随机表达a,b和γ原钙粘蛋白(Pcdh)蛋白的独特组成部分,这些蛋白在神经回路组装中起作用。我们报告说,簇状Pcdhs的所有三个亚家族都可以参与特定的同源相互作用,Pcdhα亚型的细胞表面传递需要与其他Pcdhs的顺式相互作用,而细胞外钙粘蛋白结构域EC6在此过程中起关键作用。多个Pcdh亚型的特定组合之间的同源相互作用的检查表明,Pcdh组合识别特异性取决于所有表达的亚型的身份。单个不匹配的Pcdh同工型可能会干扰这些组合的亲核相互作用。理论分析表明,Pcdh同工型组装成多聚体识别单元,并且观察到的对错配同工型的耐受性可以产生足以用于单细胞鉴定的细胞表面多样性。但是,非自我歧视和自我识别的竞争要求限制了同源识别单元发挥作用的机制。

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