Uchil Pradeep D, Quinlan Brian D, Chan Wai-Tsing, Luna Joseph M, Mothes Walther
Section of Microbial Pathogenesis, Yale University School of Medicine, New Haven, Connecticut, United States of America.
PLoS Pathog. 2008 Feb 8;4(2):e16. doi: 10.1371/journal.ppat.0040016.
Members of the TRIpartite interaction Motif (TRIM) family of E3 ligases have been shown to exhibit antiviral activities. Here we report a near comprehensive screen for antiretroviral activities of 55 TRIM proteins (36 human, 19 mouse). We identified approximately 20 TRIM proteins that, when transiently expressed in HEK293 cells, affect the entry or release of human immunodeficiency virus 1 (HIV), murine leukemia virus (MLV), or avian leukosis virus (ALV). While TRIM11 and 31 inhibited HIV entry, TRIM11 enhanced N-MLV entry by interfering with Ref1 restriction. Strikingly, many TRIM proteins affected late stages of the viral life cycle. Gene silencing of endogenously expressed TRIM 25, 31, and 62 inhibited viral release indicating that they play an important role at late stages of the viral life cycle. In contrast, downregulation of TRIM11 and 15 enhanced virus release suggesting that these proteins contribute to the endogenous restriction of retroviruses in cells.
E3 连接酶的三方相互作用基序(TRIM)家族成员已被证明具有抗病毒活性。在此,我们报告了一项针对 55 种 TRIM 蛋白(36 种人类蛋白、19 种小鼠蛋白)抗逆转录病毒活性的近乎全面的筛选。我们鉴定出约 20 种 TRIM 蛋白,当它们在 HEK293 细胞中瞬时表达时,会影响人类免疫缺陷病毒 1(HIV)、鼠白血病病毒(MLV)或禽白血病病毒(ALV)的进入或释放。虽然 TRIM11 和 31 抑制 HIV 进入,但 TRIM11 通过干扰 Ref1 限制增强了 N-MLV 的进入。引人注目的是,许多 TRIM 蛋白影响病毒生命周期的后期阶段。内源性表达的 TRIM 25、31 和 62 的基因沉默抑制了病毒释放,表明它们在病毒生命周期后期发挥重要作用。相反,TRIM11 和 15 的下调增强了病毒释放,表明这些蛋白有助于细胞内逆转录病毒的内源性限制。
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