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人甲状腺素结合球蛋白 (TBG) 启动子指导肝特异性模式下高效且持续的转基因表达。

Human thyroxine binding globulin (TBG) promoter directs efficient and sustaining transgene expression in liver-specific pattern.

机构信息

Division of Pulmonary, Allergy & Critical Care Medicine, Department of Medicine, Columbia University, New York, NY 10032, USA.

出版信息

Gene. 2012 Sep 15;506(2):289-94. doi: 10.1016/j.gene.2012.07.009. Epub 2012 Jul 20.

Abstract

The liver performs a vital role in metabolic process, which makes it an attractive target organ for gene therapy. To improve the effects of gene therapy in disorders caused by metabolic disturbance, we quantitatively evaluated six promoters, CMV, EF1α, PGK, apoE, thyroxine binding globulin (TBG), and cytochrome P450 2E1 (CYP2E1) by measuring the expression of α1-antitrypsin, which is controlled by these promoters and introduced via a lentivirus-mediated delivery system in the liver. The results showed that the TBG promoter presents as highly active though in general it is slightly lower than the ubiquitous CMV and EF1α. The expression of exogenous genes driven by the TBG promoter demonstrates to be much higher than by PGK, apoE, and CYP2E1 promoters, and the fragment of -435bp to -26bp from transcription start site (TSS) in the TBG promoter region is identified as the optimum region to direct transgene expression at a higher level. In addition, we further confirmed that the TBG promoter confers transgene persistent and specific expression within the liver up to several months after integration. The data suggests that the TBG promoter is a valuable tool and will greatly facilitate the optimization of vector design in hepatic gene therapy.

摘要

肝脏在新陈代谢过程中起着至关重要的作用,这使其成为基因治疗的理想靶器官。为了提高代谢紊乱引起的疾病的基因治疗效果,我们通过测量受这些启动子控制并通过慢病毒介导的传递系统引入肝脏的α1-抗胰蛋白酶的表达,定量评估了 6 种启动子,即 CMV、EF1α、PGK、载脂蛋白 E(apoE)、甲状腺素结合球蛋白(TBG)和细胞色素 P450 2E1(CYP2E1)。结果表明,尽管TBG 启动子通常略低于普遍存在的 CMV 和 EF1α,但它表现出高度活跃。由 TBG 启动子驱动的外源基因的表达明显高于 PGK、apoE 和 CYP2E1 启动子,并且在 TBG 启动子区域从转录起始位点(TSS)到-435bp 至-26bp 的片段被鉴定为在更高水平上指导转基因表达的最佳区域。此外,我们进一步证实,TBG 启动子在整合后几个月内可在肝脏中持续且特异性地表达转基因。数据表明,TBG 启动子是一种有价值的工具,将极大地促进肝基因治疗中载体设计的优化。

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