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酰基辅酶 A 结合聚酮化合物在 pactamycin 生物合成过程中的糖基化。

Glycosylation of acyl carrier protein-bound polyketides during pactamycin biosynthesis.

机构信息

Department of Pharmaceutical Sciences, Oregon State University, Corvallis, OR, USA.

Department of Chemistry, Oregon State University, Corvallis, OR, USA.

出版信息

Nat Chem Biol. 2019 Aug;15(8):795-802. doi: 10.1038/s41589-019-0314-6. Epub 2019 Jul 15.

Abstract

Glycosylation is a common modification reaction in natural product biosynthesis and has been known to be a post-assembly line tailoring process in glycosylated polyketide biosynthesis. Here, we show that in pactamycin biosynthesis, glycosylation can take place on an acyl carrier protein (ACP)-bound polyketide intermediate. Using in vivo gene inactivation, chemical complementation and in vitro pathway reconstitution, we demonstrate that the 3-aminoacetophenone moiety of pactamycin is derived from 3-aminobenzoic acid by a set of discrete polyketide synthase proteins via a 3-(3-aminophenyl)3-oxopropionyl-ACP intermediate. This ACP-bound intermediate is then glycosylated by an N-glycosyltransferase, PtmJ, providing a sugar precursor for the formation of the aminocyclopentitol core structure of pactamycin. This is the first example of glycosylation of a small molecule while tethered to a carrier protein. Additionally, we demonstrate that PtmO is a hydrolase that is responsible for the release of the ACP-bound product to a free β-ketoacid that subsequently undergoes decarboxylation.

摘要

糖基化是天然产物生物合成中常见的修饰反应,已知是糖基化聚酮生物合成中的装配线后修饰过程。在这里,我们表明在 pactamycin 生物合成中,糖基化可以发生在酰基辅酶 A(ACP)结合的聚酮中间产物上。通过体内基因失活、化学互补和体外途径重建,我们证明 pactamycin 的 3-氨基苯乙酮部分来自 3-氨基苯甲酸,通过一系列离散的聚酮合酶蛋白,通过 3-(3-氨基苯基)3-氧代丙酰基-ACP 中间产物。然后,该 ACP 结合的中间产物被 N-糖基转移酶 PtmJ 糖基化,为 pactamycin 的氨基环戊醇核心结构的形成提供糖前体。这是小分子与载体蛋白连接时发生糖基化的第一个例子。此外,我们证明 PtmO 是一种水解酶,负责释放 ACP 结合产物到游离的β-酮酸,随后该产物经历脱羧反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1f7b/6642016/7229154db60e/nihms-1530495-f0001.jpg

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