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Advances in siRNA delivery to T-cells: potential clinical applications for inflammatory disease, cancer and infection

机译:siRNA输送至T细胞的研究进展:炎性疾病,癌症和感染的潜在临床应用

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The specificity of RNAi and its ability to silence 'undruggable' targets has made inhibition of gene expression in T-cells with siRNAs an attractive potential therapeutic strategy for the treatment of inflammatory disease, cancer and infection. However, delivery of siRNAs into primary T-cells represents a major hurdle to their use as potential therapeutic agents. Recent advances in siRNA delivery through the use of electroporationucleofection, viral vectors, peptides/proteins, nanoparticles, aptamers and other agents have now enabled efficient gene silencing in primary T-cells both in vitro and in vivo. Overcoming such barriers in siRNA delivery offers exciting new prospects for directly targeting T-cells systemically with siRNAs, or adoptively transferring T-cells back into patients following ex vivo manipulation with siRNAs. In the present review, we outline the challenges in delivering siRNAs into primary T-cells and discuss the mechanism and therapeutic opportunities of each delivery method.We emphasize studies that have exploited RNAi-mediated gene silencing in T-cells for the treatment of inflammatory disease, cancer and infection using mouse models. We also discuss the potential therapeutic benefits of manipulating T-cells using siRNAs for the treatment of human diseases.
机译:RNAi的特异性及其沉默“非药物”靶标的能力已使抑制siRNA修饰T细胞中的基因表达成为治疗炎性疾病,癌症和感染的有吸引力的潜在治疗策略。但是,将siRNA传递至原代T细胞代表了将其用作潜在治疗剂的主要障碍。通过使用电穿孔/核转染,病毒载体,肽/蛋白质,纳米颗粒,适体和其他试剂在siRNA递送方面的最新进展现已使体外和体内初级T细胞中的基因有效沉默。克服siRNA传递中的此类障碍为使用siRNA全身性直接靶向T细胞,或在通过siRNA进行离体操作后将T细胞过继转移回患者中提供了令人兴奋的新前景。在本综述中,我们概述了将siRNA传递到原代T细胞中的挑战,并讨论了每种传递方法的机理和治疗机会。我们强调了利用RNAi介导的T细胞中的基因沉默来治疗炎性疾病的研究。 ,癌症和感染(使用小鼠模型)。我们还讨论了使用siRNA操纵T细胞治疗人类疾病的潜在治疗优势。

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