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光笼酪氨酸的计算氨酰-tRNA 合成酶文库设计。

Computational Aminoacyl-tRNA Synthetase Library Design for Photocaged Tyrosine.

机构信息

Institut für Chemie, Technische Universität Berlin, Müller-Breslau-Straße 10, 10623 Berlin, Germany.

Biophysikalische Chemie, Institut für Biologie, Humboldt-Universität zu Berlin, 10115 Berlin, Germany.

出版信息

Int J Mol Sci. 2019 May 11;20(9):2343. doi: 10.3390/ijms20092343.

Abstract

Engineering aminoacyl-tRNA synthetases (aaRSs) provides access to the ribosomal incorporation of noncanonical amino acids via genetic code expansion. Conventional targeted mutagenesis libraries with 5-7 positions randomized cover only marginal fractions of the vast sequence space formed by up to 30 active site residues. This frequently results in selection of weakly active enzymes. To overcome this limitation, we use computational enzyme design to generate a focused library of aaRS variants. For aaRS enzyme redesign, photocaged -nitrobenzyl tyrosine (ONBY) was chosen as substrate due to commercial availability and its diverse applications. Diversifying 17 first- and second-shell sites and performing conventional aaRS positive and negative selection resulted in a high-activity aaRS. This TyrRS variant carries ten mutations and outperforms previously reported ONBY-specific aaRS variants isolated from traditional libraries. In response to a single in-frame amber stop codon, it mediates the in vivo incorporation of ONBY with an efficiency matching that of the wild type TyrRS enzyme acylating cognate tyrosine. These results exemplify an improved general strategy for aaRS library design and engineering.

摘要

工程化氨酰-tRNA 合成酶(aaRS)为通过遗传密码扩展实现核糖体掺入非标准氨基酸提供了途径。具有 5-7 个位置随机化的常规靶向诱变文库仅涵盖多达 30 个活性位点残基形成的巨大序列空间的微不足道的部分。这通常导致选择弱活性的酶。为了克服这一限制,我们使用计算酶设计生成了 aaRS 变体的聚焦文库。对于 aaRS 酶重新设计,由于商业可用性和其多样化的应用,选择光笼化 - 硝基苄基酪氨酸(ONBY)作为底物。对 17 个第一和第二壳层位置进行多样化,并进行传统的 aaRS 正选择和负选择,得到了一种高活性的 aaRS。这种 TyrRS 变体携带十个突变,性能优于从传统文库中分离出的先前报道的 ONBY 特异性 aaRS 变体。它对单个框内琥珀终止密码子做出响应,介导 ONBY 的体内掺入,其效率与酰化同源酪氨酸的野生型 TyrRS 酶相当。这些结果例证了 aaRS 文库设计和工程的改进通用策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/00ef/6539999/b16f88fcef07/ijms-20-02343-g0A1.jpg

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