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首页> 外文期刊>Journal of Molecular Biology >Using Single-Molecule Approaches to Understand the Molecular Mechanisms of Heat-Shock Protein Chaperone Function
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Using Single-Molecule Approaches to Understand the Molecular Mechanisms of Heat-Shock Protein Chaperone Function

机译:使用单分子方法来了解热休克蛋白伴侣功能的分子机制

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摘要

The heat-shock proteins (Hsp) are a family of molecular chaperones, which collectively form a network that is critical for the maintenance of protein homeostasis. Traditional ensemble-based measurements have provided a wealth of knowledge on the function of individual Hsps and the Hsp network; however, such techniques are limited in their ability to resolve the heterogeneous, dynamic and transient interactions that molecular chaperones make with their client proteins. Single-molecule techniques have emerged as a powerful tool to study dynamic biological systems, as they enable rare and transient populations to be identified that would usually be masked in ensemble measurements. Thus, single-molecule techniques are particularly amenable for the study of Hsps and have begun to be used to reveal novel mechanistic details of their function. In this review, we discuss the current understanding of the chaperone action of Hsps and how gaps in the field can be addressed using single-molecule methods. Specifically, this review focuses on the ATP-independent small Hsps and the broader Hsp network and describes how these dynamic systems are amenable to single-molecule techniques.
机译:热休克蛋白(HSP)是分子伴侣系列,其共同形成了对维持蛋白质稳态至关重要的网络。基于传统的基于集合的测量已经为单个HSP和HSP网络的功能提供了丰富的知识;然而,这些技术的能力受到分解分子伴侣与其客户蛋白质制备的异质,动态和瞬态相互作用的能力。单分子技术已经出现为研究动态生物系统的强大工具,因为它们能够识别稀有和瞬态群体,通常在集合测量中掩盖。因此,单分子技术对于HSP的研究特别适用,并且已经开始用于揭示其功能的新机制细节。在本综述中,我们讨论了目前对HSP的伴侣作用的理解以及使用单分子方法可以解决现场的差距如何。具体而言,本综述侧重于ATP独立的小型HSP和更广泛的HSP网络,并描述了这些动态系统如何适应单分子技术。

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