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The Impact of Unprotected T Cells in RNAi-based Gene Therapy for HIV-AIDS

机译:未保护的T细胞在基于RNAi的HIV / AIDS基因治疗中的影响

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摘要

RNA interference (RNAi) is highly effective in inhibiting human immunodeficiency virus type 1 (HIV-1) replication by the expression of antiviral short hairpin RNA (shRNA) in stably transduced T-cell lines. For the development of a durable gene therapy that prevents viral escape, we proposed to combine multiple shRNAs against highly conserved regions of the HIV-1 RNA genome. The future in vivo application of such a gene therapy protocol will reach only a fraction of the T cells, such that HIV-1 replication will continue in the unmodified T cells, thereby possibly frustrating the therapy by generation of HIV-1 variants that escape from the inhibition imposed by the protected cells. We studied virus inhibition and evolution in pure cultures of shRNA-expressing cells versus mixed cell cultures of protected and unprotected T cells. The addition of the unprotected T cells indeed seems to accelerate HIV-1 evolution and escape from a single shRNA inhibitor. However, expression of three antiviral shRNAs from a single lentiviral vector prevents virus escape even in the presence of unprotected cells. These results support the idea to validate the therapeutic potential of this anti-HIV approach in appropriate in vivo models.
机译:通过在稳定转导的T细胞系中表达抗病毒短发夹RNA(shRNA),RNA干扰(RNAi)在抑制人类1型免疫缺陷病毒(HIV-1)复制中非常有效。为了开发可防止病毒逃逸的持久基因疗法,我们建议结合多种针对HIV-1 RNA基因组高度保守区域的shRNA。这种基因治疗方案的未来体内应用将仅达到T细胞的一小部分,这样HIV-1复制将在未修饰的T细胞中继续进行,从而可能通过产生从中逃逸的HIV-1变体而挫败治疗受保护细胞施加的抑制作用。我们研究了纯表达shRNA的细胞与受保护和不受保护的T细胞的混合细胞培养相比,病毒的抑制和进化。确实,未保护的T细胞的添加似乎确实加速了HIV-1的进化并从单一的shRNA抑制剂中逃脱。然而,即使在未受保护的细胞存在的情况下,从单个慢病毒载体表达三个抗病毒shRNA仍可阻止病毒逃逸。这些结果支持了在适当的体内模型中验证这种抗HIV方法的治疗潜力的想法。

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