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工程化睡眠美人转座酶将转座子整合重定向到基因之外。

Engineered Sleeping Beauty transposase redirects transposon integration away from genes.

机构信息

Transposition and Genome Engineering, Division of Medical Biotechnology, Paul Ehrlich Institute, Langen 63225, Germany.

Structural and Computational Biology Unit, European Molecular Biology Laboratory, Heidelberg 69117, Germany.

出版信息

Nucleic Acids Res. 2022 Mar 21;50(5):2807-2825. doi: 10.1093/nar/gkac092.

Abstract

The Sleeping Beauty (SB) transposon system is a popular tool for genome engineering, but random integration into the genome carries a certain genotoxic risk in therapeutic applications. Here we investigate the role of amino acids H187, P247 and K248 in target site selection of the SB transposase. Structural modeling implicates these three amino acids located in positions analogous to amino acids with established functions in target site selection in retroviral integrases and transposases. Saturation mutagenesis of these residues in the SB transposase yielded variants with altered target site selection properties. Transposon integration profiling of several mutants reveals increased specificity of integrations into palindromic AT repeat target sequences in genomic regions characterized by high DNA bendability. The H187V and K248R mutants redirect integrations away from exons, transcriptional regulatory elements and nucleosomal DNA in the human genome, suggesting enhanced safety and thus utility of these SB variants in gene therapy applications.

摘要

睡眠美人(SB)转座子系统是一种用于基因组工程的流行工具,但在治疗应用中,随机整合到基因组中会带来一定的遗传毒性风险。在这里,我们研究了氨基酸 H187、P247 和 K248 在 SB 转座酶靶位选择中的作用。结构建模表明,这三个氨基酸位于类似于逆转录病毒整合酶和转座酶中靶位选择功能确定的氨基酸的位置。对 SB 转座酶中这些残基进行饱和诱变,得到了靶位选择特性改变的变体。几种突变体的转座子整合分析揭示,整合到具有高 DNA 弯曲度的基因组区域中富含回文 AT 重复的靶序列的特异性增加。H187V 和 K248R 突变体将整合重新定向到人类基因组中的外显子、转录调控元件和核小体 DNA 之外,这表明这些 SB 变体在基因治疗应用中具有更高的安全性和实用性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/647e/8934666/d74bda8e537c/gkac092fig1.jpg

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