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[1型人类免疫缺陷病毒(HIV-1)基因组内的2'-O-甲基化如何调节其复制?]

[How do 2'-O-methylations within Human Immunodeficiency Virus type 1 (HIV-1) genome regulate its replication?].

作者信息

Decombe Alice, El-Kazzi Priscila, Nisole Sébastien, Decroly Étienne

机构信息

AFMB (Architecture et fonction des macromolécules biologiques), UMR 7257 - CNRS / Université Aix-Marseille, Marseille, France.

出版信息

Med Sci (Paris). 2024 May;40(5):421-427. doi: 10.1051/medsci/2024046. Epub 2024 May 31.

Abstract

The genomic RNA of HIV-1 is modified by epitranscriptomic modifications, including 2'-O-methylations, which are found on 17 internal positions. These methylations are added by the cellular methyltransferase FTSJ3, and have pro-viral effects, since they shield the viral genome from the detection by the innate immune sensor MDA5. In turn, the production of interferons by infected cells is reduced, limiting the expression of interferon-stimulated genes (ISGs) with antiviral activities. Moreover, 2'-O-methylations protect the HIV-1 genome from its degradation by ISG20, an interferon-induced exonuclease. Conversely, these methylations also exhibit antiviral effects, as they impede reverse-transcription in vitro or in quiescent cells, which are known to contain low nucleotide concentrations. Altogether, these observations suggest a balance between the proviral effect of 2'-O-methylations, related to the protection of the viral genome from detection by MDA5 and degradation by ISG20, and the antiviral effect, associated with the negative impact of 2'-O-methylations on the viral replication. These findings pave the way for further optimization of therapeutic RNA, by selective methylation of specific nucleotides.

摘要

HIV-1的基因组RNA会通过表观转录组修饰进行修饰,包括在17个内部位置发现的2'-O-甲基化。这些甲基化由细胞甲基转移酶FTSJ3添加,并具有病毒促进作用,因为它们可保护病毒基因组不被天然免疫传感器MDA5检测到。相应地,受感染细胞产生的干扰素减少,限制了具有抗病毒活性的干扰素刺激基因(ISG)的表达。此外,2'-O-甲基化可保护HIV-1基因组不被ISG20(一种干扰素诱导的核酸外切酶)降解。相反,这些甲基化也表现出抗病毒作用,因为它们在体外或在已知含有低核苷酸浓度的静止细胞中会阻碍逆转录。总之,这些观察结果表明,2'-O-甲基化的病毒促进作用(与保护病毒基因组不被MDA5检测到和不被ISG20降解有关)和抗病毒作用(与2'-O-甲基化对病毒复制的负面影响有关)之间存在平衡。这些发现为通过特定核苷酸的选择性甲基化进一步优化治疗性RNA铺平了道路。

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