突变的cas9转录激活因子在存在或不存在ltr特异性引导rna的情况下激活U1细胞中的HIV-1。

Matters Pub Date : 2017-01-01 Epub Date: 2017-01-12 DOI:10.19185/matters.201611000027
Veronica Kim, Brian M Mears, Bonita H Powell, Kenneth W Witwer
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引用次数: 10

摘要

CRISPR/Cas9系统已成为HIV根除领域中用于序列特异性破坏或延迟逆转的有前途的工具。热情与对脱靶宿主基因组修饰和对艾滋病毒进化的影响的担忧相平衡。在慢性HIV-1感染的U1单核细胞潜伏期模型中,我们证实了突变cas9转录激活因子和引导rna对HIV-1产生的刺激,其中两个引导rna明显比一个更有效。然而,在缺乏引导rna的情况下,也观察到显著的增加。我们鼓励继续仔细评估cas9介导方法的非序列特异性和脱靶效应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Mutant Cas9-transcriptional activator activates HIV-1 in U1 cells in the presence and absence of LTR-specific guide RNAs.

CRISPR/Cas9 systems have been advanced as promising tools in the HIV eradication armamentarium for sequence-specific disruption or latency reversal. Enthusiasm is balanced by concerns about off-target host genome modification and effects on HIV evolution. In the chronically HIV-1-infected U1 promonocytic latency model, we have confirmed stimulation of HIV-1 production by a mutant Cas9-transcriptional activator and guide RNAs with two guide RNAs apparently more potent than one. However, significant increases were also observed in the absence of guide RNAs. We encourage continued careful evaluation of non-sequence-specific and off-target effects of Cas9-mediated approaches.

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