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氨酰基-SNACs作为非核糖体肽合成酶缩合结构域的小分子底物。

Aminoacyl-SNACs as small-molecule substrates for the condensation domains of nonribosomal peptide synthetases.

作者信息

Ehmann D E, Trauger J W, Stachelhaus T, Walsh C T

机构信息

Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, Boston, MA 02115, USA.

出版信息

Chem Biol. 2000 Oct;7(10):765-72. doi: 10.1016/s1074-5521(00)00022-3.

Abstract

BACKGROUND

Nonribosomal peptide synthetases (NRPSs) are large multidomain proteins that catalyze the formation of a wide range of biologically active natural products. These megasynthetases contain condensation (C) domains that catalyze peptide bond formation and chain elongation. The natural substrates for C domains are biosynthetic intermediates that are covalently tethered to thiolation (T) domains within the synthetase by thioester linkages. Characterizing C domain substrate specificity is important for the engineered biosynthesis of new compounds.

RESULTS

We synthesized a series of aminoacyl-N-acetylcysteamine thioesters (aminoacyl-SNACs) and show that they are small-molecule substrates for NRPS C domains. Comparison of rates of peptide bond formation catalyzed by the C domain from enterobactin synthetase with various aminoacyl-SNACs as downstream (acceptor) substrates revealed high selectivity for the natural substrate analog L-Ser-SNAC. Comparing L- and D-Phe-SNACs as upstream (donor) substrates for the first C domain from tyrocidine synthetase revealed clear D- versus L-selectivity.

CONCLUSIONS

Aminoacyl-SNACs are substrates for NRPS C domains and are useful for characterizing the substrate specificity of C domain-catalyzed peptide bond formation.

摘要

背景

非核糖体肽合成酶(NRPSs)是大型多结构域蛋白,可催化多种生物活性天然产物的形成。这些巨型合成酶包含催化肽键形成和链延伸的缩合(C)结构域。C结构域的天然底物是通过硫酯键与合成酶内的硫醇化(T)结构域共价连接的生物合成中间体。表征C结构域底物特异性对于新化合物的工程生物合成很重要。

结果

我们合成了一系列氨酰基-N-乙酰半胱胺硫酯(氨酰基-SNACs),并表明它们是NRPS C结构域的小分子底物。用各种氨酰基-SNACs作为下游(受体)底物,比较肠杆菌素合成酶的C结构域催化的肽键形成速率,发现对天然底物类似物L-Ser-SNAC具有高选择性。比较L-和D-Phe-SNACs作为短杆菌酪肽合成酶第一个C结构域的上游(供体)底物,发现了明显的D型与L型选择性。

结论

氨酰基-SNACs是NRPS C结构域的底物,可用于表征C结构域催化的肽键形成的底物特异性。

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