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氨酰 - tRNA合成酶对辅酶A和泛酰巯基乙胺的氨酰化作用:非编码肽合成与编码肽合成之间的可能联系。

Aminoacylation of coenzyme A and pantetheine by aminoacyl-tRNA synthetases: possible link between noncoded and coded peptide synthesis.

作者信息

Jakubowski H

机构信息

Department of Microbiology and Molecular Genetics, UMDNJ-New Jersey Medical School, 185 South Orange Avenue, Newark, New Jersey 07103, USA.

出版信息

Biochemistry. 1998 Apr 14;37(15):5147-53. doi: 10.1021/bi972528v.

Abstract

Isoleucyl-tRNA synthetase (IleRS) catalyzes transfer of isoleucine from the enzyme-bound Ile-AMP and Ile-tRNA to the thiol group of coenzyme A, forming a thioester, Ile-S-CoA. Identity of Ile-S-CoA has been confirmed by several enzymatic and chemical tests. The synthesis of Ile-S-CoA, like the synthesis of other isoleucyl thioesters, is strongly shifted toward products. Other aminoacyl-tRNA synthetases, such as MetRS, AspRS, and SerRS also use CoA-SH as an acceptor for their cognate amino acids. Pantetheine also serves as an amino acid acceptor in reactions catalyzed by AspRS, IleRS, and MetRS, forming corresponding aminoacyl-S-pantetheine thioesters. It appears that CoA-SH reacts with activated amino acids by binding to each synthetase at a site, separate from the tRNA and ATP binding sites, that includes the thiol-binding subsite. These and other data support a hypothesis that the present-day aminoacyl-tRNA synthetases have originated from ancestral forms that were involved in noncoded thioester-dependent peptide synthesis, functionally similar to the present-day nonribosomal peptide synthesis by multi-enzyme thiotemplate systems.

摘要

异亮氨酰 - tRNA合成酶(IleRS)催化异亮氨酸从酶结合的Ile - AMP和Ile - tRNA转移至辅酶A的硫醇基团,形成硫酯Ile - S - CoA。Ile - S - CoA的身份已通过多项酶促和化学测试得以确认。Ile - S - CoA的合成,如同其他异亮氨酰硫酯的合成一样,强烈倾向于生成产物。其他氨酰 - tRNA合成酶,如甲硫氨酰 - tRNA合成酶(MetRS)、天冬氨酰 - tRNA合成酶(AspRS)和丝氨酰 - tRNA合成酶(SerRS),也将辅酶A - SH用作其相应氨基酸的受体。泛酰巯基乙胺在AspRS、IleRS和MetRS催化的反应中也作为氨基酸受体,形成相应的氨酰 - S - 泛酰巯基乙胺硫酯。似乎辅酶A - SH通过与每种合成酶上一个与tRNA和ATP结合位点分开的位点结合来与活化氨基酸反应,该位点包括硫醇结合亚位点。这些及其他数据支持这样一种假说,即当今的氨酰 - tRNA合成酶起源于参与非编码硫酯依赖性肽合成的祖先形式,其功能类似于当今由多酶硫醇模板系统进行的非核糖体肽合成。

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