Evaluation of HBV promoters for use in hepatic gene therapy.

P Löser, V Sandig, I Kirillova, M Strauss
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引用次数: 22

Abstract

Strategies for in vivo hepatic gene therapy will require regulatory elements which allow for long-term expression of therapeutic genes and restriction of expression to hepatocytes. This study investigates the suitability of promoters derived from hepatitis B virus (HBV) for liver-specific gene expression in vectors for hepatic gene therapy. We provide three hepatocyte-specific promoters, the HBV core promoter, the HBV core promoter linked directly to the HBV enhancer I, and a hybrid promoter containing the HBV enhancer II and a basic CMV promoter, which are hepatocyte-specific and allow for increasing levels of reporter gene expression. Moreover, in long-term expression studies using our promoter constructs in the context of an EBV based expression system we found that expression from these promoters remained nearly unchanged over a period of at least two months in hepatocyte-derived cell lines.

HBV启动子在肝脏基因治疗中的应用评估。
体内肝脏基因治疗的策略将需要允许治疗基因长期表达和限制肝细胞表达的调控元件。本研究探讨了乙型肝炎病毒(HBV)启动子在肝脏基因治疗载体中表达肝脏特异性基因的适用性。我们提供了三种肝细胞特异性启动子,HBV核心启动子,直接连接到HBV增强子I的HBV核心启动子,以及包含HBV增强子II和基本CMV启动子的混合启动子,它们是肝细胞特异性的,允许增加报告基因表达水平。此外,在基于EBV的表达系统中使用我们的启动子构建的长期表达研究中,我们发现这些启动子的表达在肝细胞来源的细胞系中至少两个月的时间内几乎保持不变。
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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