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DNA结合特异性是锌指核酸酶活性和毒性的主要决定因素。

DNA-binding Specificity Is a Major Determinant of the Activity and Toxicity of Zinc-finger Nucleases.

作者信息

Cornu Tatjana I, Thibodeau-Beganny Stacey, Guhl Eva, Alwin Stephen, Eichtinger Magdalena, Joung J K, Cathomen Toni

机构信息

Charité Medical School, Institute of Virology (CBF), Berlin, Germany.

Molecular Pathology Unit, Center for Cancer Research, and Center for Computational and Integrative Biology, Massachusetts General Hospital, Charlestown, Massachusetts, USA.

出版信息

Mol Ther. 2008 Feb;16(2):352-358. doi: 10.1038/sj.mt.6300357. Epub 2016 Dec 7.

Abstract

The engineering of proteins to manipulate cellular genomes has developed into a promising technology for biomedical research, including gene therapy. In particular, zinc-finger nucleases (ZFNs), which consist of a nonspecific endonuclease domain tethered to a tailored zinc-finger (ZF) DNA-binding domain, have proven invaluable for stimulating homology-directed gene repair in a variety of cell types. However, previous studies demonstrated that ZFNs could be associated with significant cytotoxicity due to cleavage at off-target sites. Here, we compared the in vitro affinities and specificities of nine ZF DNA-binding domains with their performance as ZFNs in human cells. The results of our cell-based assays reveal that the DNA-binding specificity-in addition to the affinity-is a major determinant of ZFN activity and is inversely correlated with ZFN-associated toxicity. In addition, our data provide the first evidence that engineering strategies, which account for context-dependent DNA-binding effects, yield ZFs that function as highly efficient ZFNs in human cells.

摘要

对蛋白质进行工程改造以操控细胞基因组,已发展成为一种用于生物医学研究(包括基因治疗)的颇具前景的技术。特别是锌指核酸酶(ZFN),它由一个与定制的锌指(ZF)DNA结合结构域相连的非特异性核酸内切酶结构域组成,已被证明在多种细胞类型中刺激同源定向基因修复方面具有极高价值。然而,先前的研究表明,由于在脱靶位点的切割,ZFN可能与显著的细胞毒性相关。在此,我们比较了九个ZF DNA结合结构域的体外亲和力和特异性,以及它们在人类细胞中作为ZFN的性能。我们基于细胞的分析结果表明,除了亲和力之外,DNA结合特异性是ZFN活性的主要决定因素,并且与ZFN相关毒性呈负相关。此外,我们的数据首次证明,考虑到上下文依赖性DNA结合效应的工程策略,能够产生在人类细胞中作为高效ZFN发挥作用的ZF。

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