首页> 美国卫生研究院文献>Cell Stress Chaperones >Sequence analyses reveal that a TPR–DP module surrounded by recombinable flanking introns could be at the origin of eukaryotic Hop and Hip TPR–DP domains and prokaryotic GerD proteins
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Sequence analyses reveal that a TPR–DP module surrounded by recombinable flanking introns could be at the origin of eukaryotic Hop and Hip TPR–DP domains and prokaryotic GerD proteins

机译:序列分析表明TPR-DP模块被重组侧翼内含子包围可能是真核Hop和Hip TPR-DP结构域以及原核GerD蛋白的起源

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摘要

The co-chaperone Hop [heat shock protein (HSP) organising protein] is known to bind both Hsp70 and Hsp90. Hop comprises three repeats of a tetratricopeptide repeat (TPR) domain, each consisting of three TPR motifs. The first and last TPR domains are followed by a domain containing several dipeptide (DP) repeats called the DP domain. These analyses suggest that the hop genes result from successive recombination events of an ancestral TPR–DP module. From a hydrophobic cluster analysis of homologous Hop protein sequences derived from gene families, we can postulate that shifts in the open reading frames are at the origin of the present sequences. Moreover, these shifts can be related to the presence or absence of biological function. We propose to extend the family of Hop co-chaperons into the kingdom of bacteria, as several structurally related genes have been identified by hydrophobic cluster analysis. We also provide evidence of common structural characteristics between hop and hip genes, suggesting a shared precursor of ancestral TPR–DP domains.Electronic supplementary materialThe online version of this article (doi:10.1007/s12192-008-0083-8) contains supplementary material, which is available to authorized users.
机译:伴侣伴侣Hop [热激蛋白(HSP)组织蛋白]已知可以结合Hsp70和Hsp90。跃点包含四肽重复(TPR)域的三个重复,每个重复由三个TPR基序组成。第一个和最后一个TPR结构域后面是一个包含几个二肽(DP)重复序列的结构域,称为DP结构域。这些分析表明,跳跃基因是由祖先TPR-DP模块的连续重组事件产生的。通过对源自基因家族的同源Hop蛋白序列的疏水聚类分析,我们可以假设开放阅读框中的移位是本序列的起源。此外,这些变化可能与生物学功能的存在与否有关。我们建议将Hop伴侣分子家族扩展到细菌界,因为已经通过疏水聚类分析确定了几种结构相关的基因。我们还提供了啤酒花和臀部基因之间共同结构特征的证据,表明了祖先TPR-DP域的共享前体。电子补充材料本文的在线版本(doi:10.1007 / s12192-008-0083-8)包含补充材料,可供授权用户使用。

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