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层粘连蛋白γ-1基因沉默可阻断克氏锥虫感染。

Silencing of the laminin gamma-1 gene blocks Trypanosoma cruzi infection.

作者信息

Nde Pius N, Simmons Kaneatra J, Kleshchenko Yuliya Y, Pratap Siddharth, Lima Maria F, Villalta Fernando

机构信息

Division of Microbial Pathogenesis and Immune Response, Department of Biomedical Sciences, School of Medicine, Meharry Medical College, 1005 Dr. D. B. Todd Jr. Blvd., Nashville, TN 37208, USA.

出版信息

Infect Immun. 2006 Mar;74(3):1643-8. doi: 10.1128/IAI.74.3.1643-1648.2006.

DOI:10.1128/IAI.74.3.1643-1648.2006
PMID:16495535
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1418675/
Abstract

It is thought that Trypanosoma cruzi, the protozoan that causes Chagas' disease, modulates the extracellular matrix network to facilitate infection of human cells. However, direct evidence to document this phenomenon is lacking. Here we show that the T. cruzi gp83 ligand, a cell surface trans-sialidase-like molecule that the parasite uses to attach to host cells, increases the level of laminin gamma-1 transcript and its expression in mammalian cells, leading to an increase in cellular infection. Stable RNA interference (RNAi) with host cell laminin gamma-1 knocks down the levels of laminin gamma-1 transcript and protein expression in mammalian cells, causing a dramatic reduction in cellular infection by T. cruzi. Thus, host laminin gamma-1, which is regulated by the parasite, plays a crucial role in the early process of infection. This is the first report showing that knocking down the expression of a human gene by RNAi inhibits the infection of an intracellular parasite.

摘要

据认为,导致恰加斯病的原生动物克氏锥虫会调节细胞外基质网络,以促进对人类细胞的感染。然而,缺乏记录这一现象的直接证据。在此我们表明,克氏锥虫gp83配体是一种细胞表面转唾液酸酶样分子,寄生虫利用它附着于宿主细胞,该配体会增加层粘连蛋白γ-1转录物的水平及其在哺乳动物细胞中的表达,从而导致细胞感染增加。用宿主细胞层粘连蛋白γ-1进行稳定的RNA干扰(RNAi)可降低哺乳动物细胞中层粘连蛋白γ-1转录物的水平和蛋白质表达,导致克氏锥虫对细胞的感染显著减少。因此,受寄生虫调节的宿主层粘连蛋白γ-1在感染的早期过程中起关键作用。这是第一份表明通过RNAi敲低人类基因的表达可抑制细胞内寄生虫感染的报告。

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