Department of Medicine, Division Hematology/Oncology, Feinberg School of Medicine, Northwestern University, Chicago, Illinois, USA.
Division of Infectious Diseases, Feinberg School of Medicine, Northwestern University, Chicago, Illinois, USA.
J Virol. 2023 Jul 27;97(7):e0065223. doi: 10.1128/jvi.00652-23. Epub 2023 Jun 13.
HIV-1 (HIV) infects CD4 T cells, the gradual depletion of which can lead to AIDS in the absence of antiretroviral therapy (ART). Some cells, however, survive HIV infection and persist as part of the latently infected reservoir that causes recurrent viremia after ART cessation. Improved understanding of the mechanisms of HIV-mediated cell death could lead to a way to clear the latent reservoir. Death induced by survival gene elimination (DISE), an RNA interference (RNAi)-based mechanism, kills cells through short RNAs (sRNAs) with toxic 6-mer seeds (positions 2 to 7 of sRNA). These toxic seeds target the 3' untranslated region (UTR) of mRNAs, decreasing the expression of hundreds of genes critical for cell survival. In most cells under normal conditions, highly expressed cell-encoded nontoxic microRNAs (miRNAs) block access of toxic sRNAs to the RNA-induced silencing complex (RISC) that mediates RNAi, promoting cell survival. HIV has been shown to inhibit the biogenesis of host miRNAs in multiple ways. We now report that HIV infection of cells deficient in miRNA expression or function results in enhanced RISC loading of an HIV-encoded miRNA HIV-miR-TAR-3p, which can kill cells by DISE through a noncanonical (positions 3 to 8) 6-mer seed. In addition, cellular RISC-bound sRNAs shift to lower seed viability. This also occurs after latent HIV provirus reactivation in J-Lat cells, suggesting independence of permissiveness of cells to viral infection. More precise targeting of the balance between protective and cytotoxic sRNAs could provide new avenues to explore novel cell death mechanisms that could be used to kill latent HIV. Several mechanisms by which initial HIV infection is cytotoxic to infected cells have been reported and involve various forms of cell death. Characterizing the mechanisms underlying the long-term survival of certain T cells that become persistent provirus reservoirs is critical to developing a cure. We recently discovered death induced by survival gene elimination (DISE), an RNAi-based mechanism of cell death whereby toxic short RNAs (sRNAs) containing 6-mer seed sequences (exerting 6-mer seed toxicity) targeting essential survival genes are loaded into RNA-induced silencing complex (RISC) complexes, resulting in inescapable cell death. We now report that HIV infection in cells with low miRNA expression causes a shift of mostly cellular RISC-bound sRNAs to more toxic seeds. This could prime cells to DISE and is further enhanced by the viral microRNA (miRNA) HIV-miR-TAR-3p, which carries a toxic noncanonical 6-mer seed. Our data provide multiple new avenues to explore novel cell death mechanisms that could be used to kill latent HIV.
HIV-1(HIV)感染 CD4 T 细胞,在没有抗逆转录病毒治疗(ART)的情况下,这些细胞逐渐耗竭会导致艾滋病。然而,一些细胞能够存活下来并作为潜伏感染库的一部分存在,该库在停止 ART 后会导致病毒再次出现。更好地了解 HIV 介导的细胞死亡机制可能会导致清除潜伏库的方法。通过生存基因消除(DISE)诱导的死亡是一种基于 RNA 干扰(RNAi)的机制,通过含有毒性 6 碱基种子(sRNA 的第 2 到 7 位)的短 RNA(sRNA)杀死细胞。这些毒性种子靶向 mRNA 的 3'非翻译区(UTR),降低了数百个对细胞存活至关重要的基因的表达。在正常条件下的大多数细胞中,高表达的细胞编码的非毒性 microRNA(miRNA)阻止毒性 sRNA 进入 RNA 诱导沉默复合物(RISC),从而促进细胞存活。HIV 已被证明可以通过多种方式抑制宿主 miRNA 的生物发生。我们现在报告说,细胞中 miRNA 表达或功能缺失的 HIV 感染会导致 HIV 编码的 miRNA HIV-miR-TAR-3p 的 RISC 装载增强,该 miRNA 可以通过非典型(第 3 到 8 位)6 碱基种子通过 DISE 杀死细胞。此外,细胞内 RISC 结合的 sRNA 转移到更低的种子活力。这也发生在 J-Lat 细胞中潜伏 HIV 前病毒重新激活后,这表明细胞对病毒感染的允许性与细胞的 miRNA 表达或功能缺失无关。更精确地靶向保护性和细胞毒性 sRNA 之间的平衡,可以提供新的途径来探索可能用于杀死潜伏 HIV 的新的细胞死亡机制。已经报道了几种初始 HIV 感染对感染细胞具有细胞毒性的机制,这些机制涉及各种形式的细胞死亡。阐明成为持续潜伏病毒库的某些 T 细胞长期存活的机制对于开发治愈方法至关重要。我们最近发现了由生存基因消除(DISE)诱导的细胞死亡,这是一种基于 RNAi 的细胞死亡机制,其中含有 6 碱基种子序列(发挥 6 碱基种子毒性)的毒性短 RNA(sRNA)靶向必需的生存基因,并被装载到 RNA 诱导的沉默复合物(RISC)复合物中,导致不可避免的细胞死亡。我们现在报告说,低 miRNA 表达的细胞中的 HIV 感染会导致大多数细胞内 RISC 结合的 sRNA 转移到毒性更大的种子。这可能使细胞更容易受到 DISE 的影响,并且进一步增强了病毒 miRNA(miRNA)HIV-miR-TAR-3p,它携带毒性非典型 6 碱基种子。我们的数据为探索可能用于杀死潜伏 HIV 的新的细胞死亡机制提供了多种新途径。
