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克氏锥虫 metacaspase 5 的重折叠、结构特征及 C 末端对蛋白重组产物的影响。

Refolding of metacaspase 5 from Trypanosoma cruzi, structural characterization and the influence of c-terminal in protein recombinant production.

机构信息

Structural and Computational Proteomics Laboratory, Carlos Chagas Institute, FIOCRUZ-PR, Curitiba/PR, 80320-290, Brazil.

Structural and Computational Proteomics Laboratory, Carlos Chagas Institute, FIOCRUZ-PR, Curitiba/PR, 80320-290, Brazil.

出版信息

Protein Expr Purif. 2022 Mar;191:106007. doi: 10.1016/j.pep.2021.106007. Epub 2021 Oct 30.

DOI:10.1016/j.pep.2021.106007
PMID:34728367
Abstract

Metacaspases are known to have a fundamental role in apoptosis-like, a programmed cellular death (PCD) in plants, fungi, and protozoans. The last includes several parasites that cause diseases of great interest to public health, mostly without adequate treatment and included in the neglected tropical diseases category. One of them is Trypanosoma cruzi which causes Chagas disease and has two metacaspases involved in its PCD: TcMCA3 and TcMCA5. Their roles seemed different in PCD, TcMCA5 appears as a proapoptotic protein negatively regulated by its C-terminal sequence, while TcMCA3 is described as a cell cycle regulator. Despite this, the precise role of TcMCA3 and TcMCA5 and their atomic structures remain elusive. Therefore, developing methodologies to allow investigations of those metacaspases is relevant. Herein, we produced full-length and truncated versions of TcMCA5 and applied different strategies for their folded recombinant production from E. coli inclusion bodies. Biophysical assays probed the efficacy of the production method in providing a high yield of folded recombinant TcMCA5. Moreover, we modeled the TcMCA5 protein structure using experimental restraints obtained by XLMS. The experimental design for novel methods and the final protocol provided here can guide studies with other metacaspases. The production of TcMCA5 allows further investigations as protein crystallography, HTS drug discovery to create potential therapeutic in the treatment of Chagas' disease and in the way to clarify how the PCD works in the parasite.

摘要

类天冬氨酸蛋白酶在植物、真菌和原生动物的凋亡样程序性细胞死亡(PCD)中起着重要作用。其中包括一些引起重大公共卫生兴趣的寄生虫病,这些寄生虫病大多没有适当的治疗方法,被归入被忽视的热带病类别。其中一种是克氏锥虫,它会引起恰加斯病,并且有两种参与其 PCD 的类天冬氨酸蛋白酶:TcMCA3 和 TcMCA5。它们在 PCD 中的作用似乎不同,TcMCA5 似乎是一种促凋亡蛋白,其 C 端序列负调控,而 TcMCA3 被描述为细胞周期调节剂。尽管如此,TcMCA3 和 TcMCA5 的精确作用及其原子结构仍然难以捉摸。因此,开发允许研究这些类天冬氨酸蛋白酶的方法是相关的。在这里,我们产生了 TcMCA5 的全长和截断版本,并应用了不同的策略来从大肠杆菌包涵体中折叠重组生产它们。生物物理测定法探测了生产方法提供高产量折叠重组 TcMCA5 的效果。此外,我们使用 XLMS 获得的实验限制来模拟 TcMCA5 蛋白结构。这里提供的新方法的实验设计和最终方案可以指导其他类天冬氨酸蛋白酶的研究。TcMCA5 的生产允许进一步研究,如蛋白质晶体学、HTS 药物发现,以创造治疗恰加斯病的潜在治疗方法,并阐明 PCD 在寄生虫中是如何发挥作用的。

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