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恶性疟原虫中SUMO化修饰的检测

Detection of SUMOylation in Plasmodium falciparum.

作者信息

Reiter Katherine H, Matunis Michael J

机构信息

Department of Biochemistry and Molecular Biology, Bloomberg School of Public Health, Johns Hopkins University, 615 North Wolfe St., Room W8118, Baltimore, MD, 21205, USA.

出版信息

Methods Mol Biol. 2016;1475:283-90. doi: 10.1007/978-1-4939-6358-4_19.

Abstract

Reversible protein modification by small ubiquitin-related modifiers (SUMOs) regulates many cellular processes, including transcription, protein quality control, cell division, and oxidative stress. SUMOylation is therefore essential for normal cell function and represents a potentially valuable target for the development of inhibitors of pathogenic eukaryotic organisms, including the malaria parasite, Plasmodium falciparum (Pf). The specific and essential functions of SUMOylation in Pf, however, remain largely uncharacterized. The further development of antimalarial drugs targeting SUMOylation would benefit significantly from a more detailed understanding of its functions and regulation during the parasite life cycle. The recent development of antibodies specific for Pf SUMO provides a valuable tool to study the functions and regulation of SUMOylation. In preliminary studies, we have used immunoblot analysis to demonstrate that SUMOylation levels vary significantly in parasites during different stages of the red blood cell cycle and also in response to oxidative stress. Owing to the dynamic nature of SUMOylation and to the robust activity of SUMO isopeptidases, analysis of SUMOylation in cultured Pf parasites requires a number of precautions during parasite purification and lysis. Here, we outline methods for preserving SUMO conjugates during isolation of Pf parasites from human red blood cell cultures, and for their detection by immunoblot analysis using PfSUMO-specific antibodies.

摘要

小泛素相关修饰物(SUMO)介导的可逆蛋白质修饰调控着许多细胞过程,包括转录、蛋白质质量控制、细胞分裂和氧化应激。因此,SUMO化对于正常细胞功能至关重要,并且是开发针对致病性真核生物(包括疟原虫恶性疟原虫(Pf))抑制剂的潜在有价值靶点。然而,SUMO化在Pf中的具体和重要功能在很大程度上仍未明确。更深入地了解其在寄生虫生命周期中的功能和调控,将极大地有助于进一步开发针对SUMO化的抗疟药物。最近开发的针对Pf SUMO的特异性抗体为研究SUMO化的功能和调控提供了一个有价值的工具。在初步研究中,我们利用免疫印迹分析证明,在红细胞周期的不同阶段以及对氧化应激的反应中,寄生虫中的SUMO化水平存在显著差异。由于SUMO化的动态性质以及SUMO异肽酶的强大活性,在培养的Pf寄生虫中分析SUMO化需要在寄生虫纯化和裂解过程中采取一些预防措施。在此,我们概述了在从人类红细胞培养物中分离Pf寄生虫过程中保存SUMO缀合物的方法,以及使用PfSUMO特异性抗体通过免疫印迹分析进行检测的方法。

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