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CPAF:一种寻找真正底物的衣原体蛋白酶。

CPAF: a Chlamydial protease in search of an authentic substrate.

机构信息

Department of Microbiology and Molecular Genetics, University of California at Irvine, Irvine, California, USA.

出版信息

PLoS Pathog. 2012;8(8):e1002842. doi: 10.1371/journal.ppat.1002842. Epub 2012 Aug 2.

Abstract

Bacteria in the genus Chlamydia are major human pathogens that cause an intracellular infection. A chlamydial protease, CPAF, has been proposed as an important virulence factor that cleaves or degrades at least 16 host proteins, thereby altering multiple cellular processes. We examined 11 published CPAF substrates and found that there was no detectable proteolysis when CPAF activity was inhibited during cell processing. We show that the reported proteolysis of these putative CPAF substrates was due to enzymatic activity in cell lysates rather than in intact cells. Nevertheless, Chlamydia-infected cells displayed Chlamydia-host interactions, such as Golgi reorganization, apoptosis resistance, and host cytoskeletal remodeling, that have been attributed to CPAF-dependent proteolysis of host proteins. Our findings suggest that other mechanisms may be responsible for these Chlamydia-host interactions, and raise concerns about all published CPAF substrates and the proposed roles of CPAF in chlamydial pathogenesis.

摘要

衣原体属细菌是主要的人类病原体,可引起细胞内感染。衣原体蛋白酶 CPAF 被认为是一种重要的毒力因子,可切割或降解至少 16 种宿主蛋白,从而改变多种细胞过程。我们研究了 11 种已发表的 CPAF 底物,发现当细胞处理过程中抑制 CPAF 活性时,没有检测到明显的蛋白水解。我们表明,这些推定的 CPAF 底物的报道蛋白水解是由于细胞裂解物中的酶活性,而不是完整细胞中的酶活性。尽管如此,感染衣原体的细胞仍显示出衣原体与宿主的相互作用,如高尔基体重组、抗细胞凋亡和宿主细胞骨架重塑,这些作用归因于依赖 CPAF 的宿主蛋白的蛋白水解。我们的研究结果表明,其他机制可能负责这些衣原体与宿主的相互作用,并对所有已发表的 CPAF 底物和 CPAF 在衣原体发病机制中的作用提出了质疑。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4a9e/3410858/f90a5ac1ec87/ppat.1002842.g001.jpg

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