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疟原虫细胞质局部 Hsp110 伴侣蛋白的独特连接片段的特征。

Characterisation of a unique linker segment of the Plasmodium falciparum cytosol localised Hsp110 chaperone.

机构信息

Department of Biochemistry, University of Venda, Private Bag X5050, Thohoyandou, 0950, South Africa; Department of Medicine, Faculty of Health Sciences, University of Cape Town, Cape Town, South Africa.

Department of Biochemistry, University of Venda, Private Bag X5050, Thohoyandou, 0950, South Africa.

出版信息

Int J Biol Macromol. 2021 Jun 1;180:272-285. doi: 10.1016/j.ijbiomac.2021.03.056. Epub 2021 Mar 16.

DOI:10.1016/j.ijbiomac.2021.03.056
PMID:33741370
Abstract

Plasmodium falciparum expresses two essential cytosol localised chaperones; PfHsp70-1 and PfHsp70-z. PfHsp70-z (Hsp110 homologue) is thought to facilitate nucleotide exchange function of PfHsp70-1. PfHsp70-1 is a refoldase, while PfHsp70-z is restricted to holdase chaperone function. The structural features delineating functional specialisation of these chaperones remain unknown. Notably, PfHsp70-z possesses a unique linker segment which could account for its distinct functions. Using recombinant forms of PfHsp70-1, PfHsp70-z and E. coli Hsp70 (DnaK) as well as their linker switch mutant forms, we explored the effects of the linker mutations by conducting several assays such as circular dichroism, intrinsic and extrinsic fluorescence coupled to biochemical and in cellular analyses. Our findings demonstrate that the linker of PfHsp70-z modulates global conformation of the chaperone, regulating several functions such as client protein binding, chaperone- and ATPase activities. In addition, as opposed to the flexible linker of PfHsp70-1, the PfHsp70-z linker is rigid, thus regulating its notable thermal stability, making it an effective stress buffer. Our findings suggest a crucial role for the linker in streamlining the functions of these two chaperones. The findings further explain how these distinct chaperones cooperate to ensure survival of P. falciparum particularly under the stressful human host environment.

摘要

疟原虫表达两种必需的细胞质定位伴侣蛋白;PfHsp70-1 和 PfHsp70-z。PfHsp70-z(Hsp110 同源物)被认为有助于 PfHsp70-1 的核苷酸交换功能。PfHsp70-1 是一种重折叠酶,而 PfHsp70-z 仅限于持家伴侣蛋白功能。这些伴侣蛋白功能特化的结构特征尚不清楚。值得注意的是,PfHsp70-z 具有独特的连接段,这可能解释了其独特的功能。我们使用重组 PfHsp70-1、PfHsp70-z 和大肠杆菌 Hsp70(DnaK)以及它们的连接开关突变体形式,通过进行圆二色性、内在和外在荧光与生化和细胞分析等几种测定来探索连接突变的影响。我们的研究结果表明,PfHsp70-z 的连接段调节伴侣蛋白的整体构象,调节几种功能,如客户蛋白结合、伴侣蛋白和 ATP 酶活性。此外,与 PfHsp70-1 的柔性连接段相反,PfHsp70-z 的连接段是刚性的,从而调节其显著的热稳定性,使其成为有效的应激缓冲剂。我们的研究结果表明,连接段在简化这两种伴侣蛋白的功能方面起着关键作用。这些发现进一步解释了这些不同的伴侣蛋白如何合作以确保疟原虫的存活,特别是在人类宿主环境的应激下。

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