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RETROVIRAL GENE THERAPY VECTORS INCLUDING INSULATOR ELEMENTS TO PROVIDE HIGH LEVELS OF GENE EXPRESSION

机译:含绝缘子的逆转录基因治疗载体可提供高水平的基因表达

摘要

Silencing of retrovirus vectors poses a significant obstacle to stem cell gene therapy, and may also impact stem cell marking and genetic manipulation studies. Retrovirus silencing is ameliorated but not eliminated by self-inactivating (SIN) mutations. The invention relates to a novel mammalian silencer-blocking assay to overcome residual silencing using insulator elements. A human β-globin transgene regulated by the Locus Control Region is silenced in transgenic mice when linked to retrovirus vector sequences. Dimer cHS4 core insulators flanking the β-globin reporter completely block MSCV retrovirus silencing in transgenic mice. This distinguishes silencer-blocking activity by cHS4 from its enhancer-blocking activity. Retrovirus vectors cannot be created at high titer with two internal dimer cHS4 cores. However, transgenic mouse silencer-blocking assays demonstrate that a combination of internal gypsy and dimer cHS4 cores cooperate to attenuate retrovirus silencing. EGFP retrovirus vectors with gypsy and the dimer cHS4 core increase expression from MSCV transduced F9 Embryonic Carcinoma cells. The highest EGFP expression in F9 cells was produced by a high titer SIN retrovirus with gypsy in the LTRs. The silencer-blocking assay described here complements current enhancer-blocking and position-effect blocking assays. The gypsy insulated SIN retrovirus vector is particularly well suited for gene therapy and for stem cell marking studies.
机译:逆转录病毒载体的沉默对干细胞基因治疗构成了重大障碍,也可能影响干细胞标记和基因操作研究。逆转录病毒沉默得到改善,但不能通过自灭活(SIN)突变消除。本发明涉及一种新颖的哺乳动物消音器阻滞测定法,以克服使用绝缘体元件的残留沉默。当与逆转录病毒载体序列连接时,由基因座控制区调节的人β-珠蛋白转基因在转基因小鼠中沉默。 β-珠蛋白报道基因两侧的二聚体cHS4核心绝缘子完全阻断了转基因小鼠中的MSCV逆转录病毒沉默。这将cHS4的沉默子阻断活性与其增强子阻断活性区分开来。不能使用两个内部二聚体cHS4核心以高滴度创建逆转录病毒载体。但是,转基因小鼠沉默抑制试验表明,内部吉普赛人和二聚体cHS4核的组合可减弱逆转录病毒沉默。具有吉普赛人和二聚体cHS4核心的EGFP逆转录病毒载体可提高MSCV转导的F9胚胎癌细胞的表达。 F9细胞中EGFP的最高表达是由高滴度的SIN逆转录病毒在LTR中具有吉普赛人产生的。本文所述的消音剂阻断测定法是对当前增强剂阻断剂和位置效应阻断剂测定法的补充。吉普赛绝缘SIN逆转录病毒载体特别适合基因治疗和干细胞标记研究。

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