首页> 外文期刊>Philosophical Transactions of the Royal Society of London, Series B. Biological Sciences >Use of a coenzyme by the glmS ribozymeriboswitch suggests primordial expansion of RNA chemistry by small molecules
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Use of a coenzyme by the glmS ribozymeriboswitch suggests primordial expansion of RNA chemistry by small molecules

机译:glmS核糖转移酶开关对辅酶的使用表明小分子对RNA化学的原始扩展

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摘要

The glmS ribozyme-riboswitch is the first known example of a naturally occurring catalytic RNA that employs a small molecule as a coenzyme. Binding of glucosamine-6-phosphate (GlcN6P) activates self-cleavage of the bacterial ribozyme, which is part of the mRNA encoding the metabolic enzyme GlcN6P-synthetase. Cleavage leads to negative feedback regulation. GlcN6P binds in the active site of the ribozyme, where its amine could function as a general acid and electrostatic catalyst. The ribozyme is pre-folded but inactive in the absence of GlcN6P, demonstrating it has evolved strict dependence on the exogenous small molecule. The ribozyme showcases the ability of RNA to co-opt non-covalently bound smallmolecules to expand its chemical repertoire. Analogue studies demonstrate that some molecules other than GlcN6P, such as L-serine (but not D-serine), can function as weak activators. This suggests how coenzyme use by RNA world ribozymes may have led to evolution of proteins. Primordial cofactor-dependent ribozymes may have evolved to bind their cofactors covalently. If amino acids were used as cofactors, this could have driven the evolution ofRNA aminoacylation. The ability to make covalently bound peptide coenzymes may have further increased the fitness of such primordial ribozymes, providing a selective pressure for the invention of translation.
机译:glmS核酶-核糖开关是采用小分子作为辅酶的天然催化RNA的第一个已知实例。 6-磷酸氨基葡萄糖的结合(GlcN6P)激活细菌核酶的自切割,该酶是编码代谢酶GlcN6P合成酶的mRNA的一部分。分裂导致负反馈调节。 GlcN6P结合在核酶的活性位点上,在那里它的胺可以充当一般的酸和静电催化剂。核酶是预先折叠的,但是在没有GlcN6P的情况下却没有活性,表明核酶已经严格依赖于外源小分子。核酶展示了RNA共选择非共价结合的小分子以扩展其化学组成的能力。类比研究表明,除GlcN6P以外的某些分子,例如L-丝氨酸(而不是D-丝氨酸)可以充当弱激活剂。这表明RNA世界核酶如何利用辅酶可能导致蛋白质进化。原始辅因子依赖性核酶可能已经进化为共价结合其辅因子。如果将氨基酸用作辅助因子,则可能已经推动了RNA氨酰化的发展。制备共价结合的肽辅酶的能力可能进一步提高了这种原始核酶的适应性,为翻译的发明提供了选择压力。

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