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P58~(IPK), a novel cochaperone containing tetratricopeptide repeats and a J-domain with oncogenic potential

机译:P58〜(IPK),一种含有四肽重复序列和具有致癌潜能的J结构域的新型伴侣蛋白

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摘要

Tetratricopeptide repeats (TPRs) are loosely conserved 34-amino acid sequence motifs that have been shown to function as scaffolding structures to mediate protein-protein interactions. TPRs have been identified in a number of proteins with diverse functions and cellular locations. Recent studies suggest that individual TPR motifs can confer specificity in promoting homotypic and/or heterotypic interactions, often in a mutually exclusive manner. These features are best exemplified by the P58~(IPK) protein, an influenza virus-activated cellular inhibitor of the PKR protein kinase, whose different TRP motifs mediate interactions with distinct proteins. P58~(IPK), which possesses cochaperone and oncogenic properties, represents a unique class of TPR proteins containing a J-domain. Here we review recent progress on the structural and functional characterization of P58~(IPK), and discuss the possible mechanisms by which P58~(IPK), modulates PKR and induces tumorigenesis in view of present knowledge of TPR proteins and molecular chaperones.
机译:四肽重复序列(TPR)是保守的34个氨基酸序列的基序,已被证明可充当支架结构来介导蛋白质-蛋白质相互作用。在许多具有不同功能和细胞位置的蛋白质中已鉴定出TPR。最近的研究表明,单个TPR基序通常可以以互斥的方式赋予促进同型和/或异型相互作用的特异性。这些特征可以通过流感病毒激活的PKR蛋白激酶细胞抑制剂P58〜(IPK)蛋白得到最好的体现,其不同的TRP基序介导与不同蛋白的相互作用。具有伴侣蛋白和致癌特性的P58〜(IPK)代表一类独特的含有J结构域的TPR蛋白。在这里,我们综述了有关P58〜(IPK)的结构和功能表征的最新进展,并根据目前对TPR蛋白和分子伴侣的了解,讨论了P58〜(IPK)调节PKR并诱导肿瘤发生的可能机制。

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