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Transcriptional Targeting and MicroRNA Regulation of Lentiviral Vectors

机译:慢病毒载体的转录靶向和微小RNA调节

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Gene expression regulation is the result of complex interactions between transcriptional and post-transcriptional controls, resulting in cell-type-specific gene expression patterns that are determined by the developmental and differentiation stage of pathophysiological conditions. Understanding the complexity of gene expression regulatory networks is fundamental to gene therapy, an approach which has the potential to treat and cure inherited disorders by delivering the correct gene to patient specific cells or tissues by means of both viral and non-viral vectors. Besides the issues of biosafety, in recent years efforts have focused on achieving a robust and sustained transgene expression, which attains a phenotypic correction in several diseases, while avoiding transgene-related adverse effects, such as overexpression-associated cytotoxicity and/or immune responses to the transgene. In this sense, the use of cell-type-specific promoters and microRNA target sequences (miRTs) in gene transfer expression cassettes have allowed for a restricted expression after gene transfer in several studies. This review will focus on the use of transcriptional and post-transcriptional regulation to achieve a highly specific and safe transgene expression, as well as their application in ex?vivo and in?vivo gene therapeutic approaches.
机译:基因表达调节是转录和转录后对照之间复杂相互作用的结果,导致细胞型特异性基因表达模式,其由病理生理病症的发育和分化阶段确定。了解基因表达调控网络的复杂性是基因治疗的基础,一种方法可以通过借助于病毒和非病毒载体将正确的基因递送患者特异性细胞或组织来治疗和治愈遗传性疾病的方法。除了生物安全问题之外,近年来努力致力于实现稳健和持续的转基因表达,该表达在几种疾病中达到了表型校正,同时避免了相关的相关不良反应,例如过表达相关的细胞毒性和/或免疫应答转基因。从这个意义上讲,在基因转移表达盒中使用细胞型特异性启动子和MicroRNA靶序列(MIRTS)在几项研究中的基因转移后允许受限制的表达。本综述将专注于使用转录和转录后调节,以达到高度特异性和安全的转基因表达,以及它们在Ex'Vivo和βvivo基因治疗方法中的应用。

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