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复杂 J 蛋白网络在真核生物中推动蛋白解聚的进化。

Evolution of an intricate J-protein network driving protein disaggregation in eukaryotes.

机构信息

Center for Molecular Biology (ZMBH), Heidelberg University, Heidelberg, Germany.

DKFZ-ZMBH Alliance, German Cancer Research Center (DKFZ), Heidelberg, Germany.

出版信息

Elife. 2017 May 15;6:e24560. doi: 10.7554/eLife.24560.

Abstract

Hsp70 participates in a broad spectrum of protein folding processes extending from nascent chain folding to protein disaggregation. This versatility in function is achieved through a diverse family of J-protein cochaperones that select substrates for Hsp70. Substrate selection is further tuned by transient complexation between different classes of J-proteins, which expands the range of protein aggregates targeted by metazoan Hsp70 for disaggregation. We assessed the prevalence and evolutionary conservation of J-protein complexation and cooperation in disaggregation. We find the emergence of a eukaryote-specific signature for interclass complexation of canonical J-proteins. Consistently, complexes exist in yeast and human cells, but not in bacteria, and correlate with cooperative action in disaggregation in vitro. Signature alterations exclude some J-proteins from networking, which ensures correct J-protein pairing, functional network integrity and J-protein specialization. This fundamental change in J-protein biology during the prokaryote-to-eukaryote transition allows for increased fine-tuning and broadening of Hsp70 function in eukaryotes.

摘要

Hsp70 参与广泛的蛋白质折叠过程,从新生链折叠到蛋白质解聚。这种多功能性是通过多种 J 蛋白共伴侣实现的,这些伴侣选择 Hsp70 的底物。通过不同类别的 J 蛋白之间的瞬时复合物形成,进一步调整了底物选择,这扩大了后生动物 Hsp70 用于解聚的蛋白质聚集体的靶标范围。我们评估了 J 蛋白在解聚中的复合物形成和合作的普遍性和进化保守性。我们发现,经典 J 蛋白的类间复合物形成出现了真核生物特有的特征。一致地,复合物存在于酵母和人类细胞中,但不存在于细菌中,并且与体外解聚中的合作作用相关。特征改变将一些 J 蛋白排除在网络之外,这确保了正确的 J 蛋白配对、功能网络完整性和 J 蛋白的专业化。在原核生物到真核生物的过渡过程中,J 蛋白生物学发生了这种根本性的变化,从而允许在后生动物中增加 Hsp70 功能的精细调整和拓宽。

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