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细胞外囊泡上调并直接传递黏附因子,促进宿主细胞定植。

extracellular vesicles up-regulate and directly transfer adherence factors promoting host cell colonization.

机构信息

Department of Microbiology, Immunology and Molecular Genetics, University of California, Los Angeles, CA 90095.

Department of Biology, San Diego State University, San Diego, CA 92182.

出版信息

Proc Natl Acad Sci U S A. 2024 Jun 18;121(25):e2401159121. doi: 10.1073/pnas.2401159121. Epub 2024 Jun 12.

Abstract

, a common sexually transmitted parasite that colonizes the human urogenital tract, secretes extracellular vesicles (TvEVs) that are taken up by human cells and are speculated to be taken up by parasites as well. While the crosstalk between TvEVs and human cells has led to insight into host:parasite interactions, roles for TvEVs in infection have largely been one-sided, with little known about the effect of TvEV uptake by . Approximately 11% of infections are found to be coinfections of multiple strains. Clinical isolates often differ in their adherence to and cytolysis of host cells, underscoring the importance of understanding the effects of TvEV uptake within the parasite population. To address this question, our lab tested the ability of a less adherent strain of , G3, to take up fluorescently labeled TvEVs derived from both itself (G3-EVs) and TvEVs from a more adherent strain of the parasite (B7RC2-EVs). Here, we showed that TvEVs generated from the more adherent strain are internalized more efficiently compared to the less adherent strain. Additionally, preincubation of G3 parasites with B7RC2-EVs increases parasite aggregation and adherence to host cells. Transcriptomics revealed that TvEVs up-regulate expression of predicted parasite membrane proteins and identified an adherence factor, heteropolysaccharide binding protein (HPB2). Finally, using comparative proteomics and superresolution microscopy, we demonstrated direct transfer of an adherence factor, cadherin-like protein, from TvEVs to the recipient parasite's surface. This work identifies TvEVs as a mediator of parasite:parasite communication that may impact pathogenesis during mixed infections.

摘要

, 一种常见的性传播寄生虫,定植于人体泌尿生殖道,分泌细胞外囊泡(TvEVs),这些囊泡被人体细胞摄取,并推测也被寄生虫摄取。虽然 TvEVs 与人体细胞之间的串扰导致了宿主-寄生虫相互作用的深入了解,但 TvEVs 在感染中的作用基本上是片面的,关于 TvEVs 被摄取对寄生虫的影响知之甚少。大约 11%的感染被发现是多种 菌株的合并感染。临床分离株在对宿主细胞的粘附和细胞溶解方面往往存在差异,这突显了了解寄生虫群体中 TvEV 摄取影响的重要性。为了解决这个问题,我们实验室测试了一种粘附性较低的 菌株 G3 摄取荧光标记的源自自身(G3-EVs)和寄生虫粘附性更强的菌株(B7RC2-EVs)的 TvEVs 的能力。在这里,我们表明,与粘附性较低的菌株相比,源自粘附性更强的菌株的 TvEVs 被更有效地内化。此外,将 G3 寄生虫与 B7RC2-EVs 预孵育会增加寄生虫聚集和对宿主细胞的粘附。转录组学显示,TvEVs 上调了预测寄生虫膜蛋白的表达,并鉴定出一种粘附因子,异多糖结合蛋白(HPB2)。最后,通过比较蛋白质组学和超分辨率显微镜,我们证明了一种粘附因子,钙粘蛋白样蛋白,从 TvEVs 直接转移到受纳寄生虫的表面。这项工作将 TvEVs 确定为寄生虫-寄生虫通讯的介质,这可能会影响混合感染期间的发病机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8c2d/11194581/e2ef9217a21e/pnas.2401159121fig01.jpg

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