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Chemical engineering of the peptidyl transferase center reveals an important role of the 2′-hydroxyl group of A2451

机译:肽基转移酶中心的化学工程揭示了A2451 2-羟基的重要作用

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摘要

The main enzymatic reaction of the large ribosomal subunit is peptide bond formation. Ribosome crystallography showed that A2451 of 23S rRNA makes the closest approach to the attacking amino group of aminoacyl-tRNA. Mutations of A2451 had relatively small effects on transpeptidation and failed to unequivocally identify the crucial functional group(s). Here, we employed an in vitro reconstitution system for chemical engineering the peptidyl transferase center by introducing non-natural nucleosides at position A2451. This allowed us to investigate the peptidyl transfer reaction performed by a ribosome that contained a modified nucleoside at the active site. The main finding is that ribosomes carrying a 2′-deoxyribose at A2451 showed a compromised peptidyl transferase activity. In variance, adenine base modifications and even the removal of the entire nucleobase at A2451 had only little impact on peptide bond formation, as long as the 2′-hydroxyl was present. This implicates a functional or structural role of the 2′-hydroxyl group at A2451 for transpeptidation.
机译:大核糖体亚基的主要酶促反应是肽键形成。核糖体晶体学表明,23S rRNA的A2451最接近攻击氨酰基tRNA的氨基。 A2451的突变对转肽作用相对较小,并且不能明确鉴定关键的功能基团。在这里,我们通过在位置A2451处引入非天然核苷,对肽基转移酶中心进行了化学工程改造,采用了体外重组系统。这使我们能够研究由在活性位点含有修饰核苷的核糖体进行的肽基转移反应。主要发现是在A2451携带2'-脱氧核糖的核糖体显示出受损的肽基转移酶活性。作为变化,只要存在2'-羟基,腺嘌呤碱基的修饰甚至在A2451的整个核碱基的去除对肽键的形成几乎没有影响。这暗示了A2451处的2'-羟基的功能或结构作用用于转肽作用。

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