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一种基于可编程核酶的用于非天然氨基酸的tRNA氨基酰化系统。

A tRNA aminoacylation system for non-natural amino acids based on a programmable ribozyme.

作者信息

Bessho Yoshitaka, Hodgson David R W, Suga Hiroaki

机构信息

Department of Chemistry, University at Buffalo, State University of New York, Buffalo, NY 14260-3000, USA.

出版信息

Nat Biotechnol. 2002 Jul;20(7):723-8. doi: 10.1038/nbt0702-723.

Abstract

The ability to recognize tRNA identities is essential to the function of the genetic coding system. In translation aminoacyl-tRNA synthetases (ARSs) recognize the identities of tRNAs and charge them with their cognate amino acids. We show that an in vitro evolved ribozyme can also discriminate between specific tRNAs, and can transfer amino acids to the 3' ends of cognate tRNAs. The ribozyme interacts with both the CCA-3' terminus and the anticodon loop of tRNA(fMet), and its tRNA specificity is controlled by these interactions. This feature allows us to program the selectivity of the ribozyme toward specific tRNAs, and therefore to tailor effective aminoacyl-transfer catalysts. This method potentially provides a means of generating aminoacyl tRNAs that are charged with non-natural amino acids, which could be incorporated into proteins through cell-free translation.

摘要

识别tRNA身份的能力对于遗传编码系统的功能至关重要。在翻译过程中,氨酰-tRNA合成酶(ARS)识别tRNA的身份并为其装载相应的氨基酸。我们发现,体外进化的核酶也能够区分特定的tRNA,并能将氨基酸转移至同源tRNA的3'末端。该核酶与tRNA(fMet)的CCA-3'末端和反密码子环相互作用,其对tRNA的特异性由这些相互作用控制。这一特性使我们能够对核酶针对特定tRNA的选择性进行编程,从而定制有效的氨酰转移催化剂。该方法有可能提供一种生成装载非天然氨基酸的氨酰tRNA的手段,这些氨酰tRNA可通过无细胞翻译整合到蛋白质中。

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