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CTF/NF1 转录因子可作为整合基因转移载体的有效遗传绝缘子。

CTF/NF1 transcription factors act as potent genetic insulators for integrating gene transfer vectors.

机构信息

Institute of Biotechnology, University of Lausanne, Lausanne, Switzerland.

出版信息

Gene Ther. 2012 Jan;19(1):15-24. doi: 10.1038/gt.2011.70. Epub 2011 May 12.

Abstract

Gene transfer-based therapeutic approaches have greatly benefited from the ability of some viral vectors to efficiently integrate within the cell genome and ensure persistent transmission of newly acquired transgenes to the target cell progeny. However, integration of provirus has been associated with epigenetic repercussions that may influence the expression of both the transgene and cellular genes close to vector integration loci. The exploitation of genetic insulator elements may overcome both issues through their ability to act as barriers that limit transgene silencing and/or as enhancer-blockers preventing the activation of endogenous genes by the vector enhancer. We established quantitative plasmid-based assay systems to screen enhancer-blocker and barrier genetic elements. Short synthetic insulators that bind to nuclear factor-I protein family transcription factors were identified to exert both enhancer-blocker and barrier functions, and were compared to binding sites for the insulator protein CTCF (CCCTC-binding factor). Gamma-retroviral vectors enclosing these insulator elements were produced at titers similar to their non-insulated counterparts and proved to be less genotoxic in an in vitro immortalization assay, yielding lower activation of Evi1 oncogene expression and reduced clonal expansion of bone marrow cells.

摘要

基于基因转移的治疗方法极大地受益于某些病毒载体能够有效地整合到细胞基因组中,并确保新获得的转基因持续传递给靶细胞后代的能力。然而,前病毒的整合与表观遗传反应有关,这可能会影响转基因和靠近载体整合位点的细胞基因的表达。通过充当限制转基因沉默和/或作为增强子阻断剂的屏障的能力,利用遗传绝缘子元件可以克服这两个问题,从而阻止载体增强子激活内源性基因。我们建立了定量质粒为基础的筛选增强子阻断剂和屏障遗传元件的测定系统。短的合成绝缘子与核因子-I 蛋白家族转录因子结合,表现出增强子阻断剂和屏障功能,并与绝缘子蛋白 CTCF(CCCTC 结合因子)的结合位点进行了比较。包含这些绝缘子元件的γ逆转录病毒载体以与非绝缘载体相似的滴度产生,并在体外永生化测定中证明毒性较小,Evi1 癌基因表达的激活降低,骨髓细胞的克隆扩增减少。

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