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首页> 外文期刊>Virology >Latently-infected CD4+ T cells are enriched for HIV-1 Tat variants with impaired transactivation activity.
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Latently-infected CD4+ T cells are enriched for HIV-1 Tat variants with impaired transactivation activity.

机译:潜在感染的CD4 + T细胞富含反式激活活性受损的HIV-1 Tat变体。

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摘要

The ability of HIV to establish latent infection in CD4+ lymphocytes represents a major barrier to the eradication of HIV. It is not clear what mechanisms favor latent over productive infection, but prior studies have suggested a role for the viral transcription factor Tat or its RNA target, TAR. Using samples from five individuals who were started on ART within 6 months of infection and achieved a viral load <50 (suppressed), we isolated one- and two-exon tat RNA from HIV propagated ex vivo from baseline plasma and from co-cultures of CD4+ T cells obtained at baseline and suppressed time points. Compared to virus from the baseline plasma (mostly from productively-infected CD4+ T cells), virus from the baseline and suppressed co-cultures (mostly from latently-infected cells) had more Tat variants with impaired transactivation activity. These findings suggest that impaired activity in the Tat-TAR axis may contribute to the establishment of latent infection in CD4+ T cells.
机译:HIV在CD4 +淋巴细胞中潜在感染的能力代表了根除HIV的主要障碍。目前尚不清楚哪种机制更有利于潜在感染而不是生产性感染,但先前的研究表明病毒转录因子Tat或其RNA靶标TAR发挥了作用。使用从感染后6个月内开始接受抗逆转录病毒治疗并达到病毒载量<50(抑制)的五个个体的样本中,我们从基线血浆中和体外共培养的HIV分离出的HIV中分离了一个和两个外显子的tat RNA。在基线和抑制的时间点获得CD4 + T细胞。与来自基线血浆的病毒(主要来自生产性感染的CD4 + T细胞)相比,来自基线和抑制的共培养物(主要来自潜伏感染的细胞)的病毒具有更多的Tat变异体,其反式激活活性受损。这些发现表明,Tat-TAR轴上的活性减弱可能有助于CD4 + T细胞中潜伏感染的建立。

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