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复制蛋白A具有典型功能,并且也参与克氏锥虫的分化能力。

Replication Protein A Presents Canonical Functions and Is Also Involved in the Differentiation Capacity of Trypanosoma cruzi.

作者信息

Pavani Raphael Souza, da Silva Marcelo Santos, Fernandes Carlos Alexandre Henrique, Morini Flavia Souza, Araujo Christiane Bezerra, Fontes Marcos Roberto de Mattos, Sant'Anna Osvaldo Augusto, Machado Carlos Renato, Cano Maria Isabel, Fragoso Stenio Perdigão, Elias Maria Carolina

机构信息

Laboratório Especial de Ciclo Celular, Instituto Butantan, São Paulo, São Paulo, Brazil.

Center of Toxins, Immune Response and Cell Signaling-CeTICS, Instituto Butantan, São Paulo, São Paulo, Brazil.

出版信息

PLoS Negl Trop Dis. 2016 Dec 16;10(12):e0005181. doi: 10.1371/journal.pntd.0005181. eCollection 2016 Dec.

Abstract

Replication Protein A (RPA), the major single stranded DNA binding protein in eukaryotes, is composed of three subunits and is a fundamental player in DNA metabolism, participating in replication, transcription, repair, and the DNA damage response. In human pathogenic trypanosomatids, only limited studies have been performed on RPA-1 from Leishmania. Here, we performed in silico, in vitro and in vivo analysis of Trypanosoma cruzi RPA-1 and RPA-2 subunits. Although computational analysis suggests similarities in DNA binding and Ob-fold structures of RPA from T. cruzi compared with mammalian and fungi RPA, the predicted tridimensional structures of T. cruzi RPA-1 and RPA-2 indicated that these molecules present a more flexible tertiary structure, suggesting that T. cruzi RPA could be involved in additional responses. Here, we demonstrate experimentally that the T. cruzi RPA complex interacts with DNA via RPA-1 and is directly related to canonical functions, such as DNA replication and DNA damage response. Accordingly, a reduction of TcRPA-2 expression by generating heterozygous knockout cells impaired cell growth, slowing down S-phase progression. Moreover, heterozygous knockout cells presented a better efficiency in differentiation from epimastigote to metacyclic trypomastigote forms and metacyclic trypomastigote infection. Taken together, these findings indicate the involvement of TcRPA in the metacyclogenesis process and suggest that a delay in cell cycle progression could be linked with differentiation in T. cruzi.

摘要

复制蛋白A(RPA)是真核生物中主要的单链DNA结合蛋白,由三个亚基组成,是DNA代谢的重要参与者,参与复制、转录、修复及DNA损伤反应。在人类致病锥虫中,对利什曼原虫的RPA-1仅进行了有限的研究。在此,我们对克氏锥虫的RPA-1和RPA-2亚基进行了计算机模拟、体外和体内分析。尽管计算分析表明,与哺乳动物和真菌的RPA相比,克氏锥虫RPA在DNA结合和Ob折叠结构上具有相似性,但克氏锥虫RPA-1和RPA-2的预测三维结构表明,这些分子呈现出更灵活的三级结构,这表明克氏锥虫RPA可能参与了其他反应。在此,我们通过实验证明,克氏锥虫RPA复合物通过RPA-1与DNA相互作用,并且与DNA复制和DNA损伤反应等经典功能直接相关。因此,通过产生杂合敲除细胞降低TcRPA-2的表达会损害细胞生长,减缓S期进程。此外,杂合敲除细胞在从无鞭毛体向循环后期锥鞭毛体形式的分化以及循环后期锥鞭毛体感染方面表现出更高的效率。综上所述,这些发现表明TcRPA参与了循环后期发育过程,并表明细胞周期进程的延迟可能与克氏锥虫的分化有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f107/5161316/6f0dba52e566/pntd.0005181.g001.jpg

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