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线粒体 Hsp70 伴侣系统在细胞存活和衰老中的相互作用的不断变化的范式。

Evolving paradigms on the interplay of mitochondrial Hsp70 chaperone system in cell survival and senescence.

机构信息

Department of Biochemistry, Indian Institute of Science, Bangalore, India.

Department of Zoology, Institute of Science, Banaras Hindu University, Varanasi, India.

出版信息

Crit Rev Biochem Mol Biol. 2019 Dec;54(6):517-536. doi: 10.1080/10409238.2020.1718062. Epub 2020 Jan 30.

Abstract

The role of mitochondria within a cell has grown beyond being the prime source of cellular energy to one of the major signaling platforms. Recent evidence provides several insights into the crucial roles of mitochondrial chaperones in regulating the organellar response to external triggers. The mitochondrial Hsp70 (mtHsp70/Mortalin/Grp75) chaperone system plays a critical role in the maintenance of proteostasis balance in the organelle. Defects in mtHsp70 network result in attenuated protein transport and misfolding of polypeptides leading to mitochondrial dysfunction. The functions of Hsp70 are primarily governed by J-protein cochaperones. Although human mitochondria possess a single Hsp70, its multifunctionality is characterized by the presence of multiple specific J-proteins. Several studies have shown a potential association of Hsp70 and J-proteins with diverse pathological states that are not limited to their canonical role as chaperones. The role of mitochondrial Hsp70 and its co-chaperones in disease pathogenesis has not been critically reviewed in recent years. We evaluated some of the cellular interfaces where Hsp70 machinery associated with pathophysiological conditions, particularly in context of tumorigenesis and neurodegeneration. The mitochondrial Hsp70 machinery shows a variable localization and integrates multiple components of the cellular processes with varied phenotypic consequences. Although Hsp70 and J-proteins function synergistically in proteins folding, their precise involvement in pathological conditions is mainly idiosyncratic. This machinery is associated with a heterogeneous set of molecules during the progression of a disorder. However, the precise binding to the substrate for a specific physiological response under a disease subtype is still an undocumented area of analysis.

摘要

细胞内线粒体的作用已经超越了作为细胞能量的主要来源,成为主要的信号平台之一。最近的证据提供了一些关于线粒体伴侣在调节细胞器对外界触发的反应方面的关键作用的见解。线粒体热休克蛋白 70(mtHsp70/Mortalin/Grp75)伴侣系统在细胞器中维持蛋白质稳态平衡方面发挥着关键作用。mtHsp70 网络的缺陷导致蛋白质转运减弱和多肽错误折叠,从而导致线粒体功能障碍。Hsp70 的功能主要由 J 蛋白共伴侣控制。尽管人类线粒体只拥有一种 Hsp70,但它的多功能性是由多种特异性 J 蛋白的存在所决定的。几项研究表明,Hsp70 和 J 蛋白与多种病理状态之间存在潜在的关联,而不仅仅局限于它们作为伴侣的典型作用。近年来,线粒体 Hsp70 及其共伴侣在疾病发病机制中的作用尚未得到批判性评估。我们评估了 Hsp70 机制与病理生理状况相关的一些细胞界面,特别是在肿瘤发生和神经退行性变的背景下。线粒体 Hsp70 机制显示出可变的定位,并整合了细胞过程的多个组件,具有不同的表型后果。尽管 Hsp70 和 J 蛋白在蛋白质折叠中协同作用,但它们在病理条件下的确切作用主要是特有的。在疾病进展过程中,这种机制与一组异质分子相关。然而,在疾病亚型下,特定生理反应的特定底物的精确结合仍然是一个未被记录的分析领域。

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