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非血红素单加氧酶 ThoJ 催化硫醇酰胺 β-羟化。

Non-Heme Monooxygenase ThoJ Catalyzes Thioholgamide β-Hydroxylation.

机构信息

Workgroup Structural Biology of Biosynthetic Enzymes, Helmholtz Institute for Pharmaceutical Research Saarland (HIPS), Helmholtz Centre for Infection Research (HZI), Saarland University, Campus Geb. E8.1, 66123 Saarbrücken, Germany.

Department Microbial Natural Products, Actinobacteria Metabolic Engineering Group, Helmholtz Institute for Pharmaceutical Research Saarland (HIPS), Helmholtz Centre for Infection Research (HZI), Saarland University, CampusC2.3, 66123 Saarbrücken, Germany.

出版信息

ACS Chem Biol. 2020 Oct 16;15(10):2815-2819. doi: 10.1021/acschembio.0c00637. Epub 2020 Oct 1.

Abstract

Thioviridamide-like compounds, including thioholgamides, are ribosomally synthesized and post-translationally modified peptide natural products with potent anticancer cell activity and an unprecedented structure. Very little is known about their biosynthesis, and we were intrigued by the β-hydroxy-N1, N3-dimethylhistidinium moiety found in these compounds. Here we report the construction of a heterologous host capable of producing thioholgamide with a 15-fold increased yield compared to the wild-type strain. A knockout of , encoding a predicted nonheme monooxygenase, shows that ThoJ is essential for thioholgamide β-hydroxylation. The crystal structure of ThoJ exhibits a typical mono/dioxygenase fold with conserved key active-site residues. Yet, ThoJ possesses a very large substrate binding pocket that appears suitable to receive a cyclic thioholgamide intermediate for hydroxylation. The improved production of the heterologous host will enable the dissection of the individual biosynthetic steps involved in biosynthesis of this exciting RiPP family.

摘要

硫苷类似物,包括硫醇霉素,是核糖体合成和翻译后修饰的肽天然产物,具有很强的抗癌细胞活性和前所未有的结构。关于它们的生物合成知之甚少,我们对这些化合物中发现的β-羟基-N1、N3-二甲基组氨酸部分很感兴趣。在这里,我们报告了一种异源宿主的构建,该宿主能够产生硫醇霉素,其产量比野生型菌株增加了 15 倍。一个编码预测的非血红素单加氧酶的基因的敲除表明,ThoJ 对硫醇霉素的β-羟化是必不可少的。ThoJ 的晶体结构显示出典型的单/双加氧酶折叠,具有保守的关键活性位点残基。然而,ThoJ 具有一个非常大的底物结合口袋,似乎适合接收环状硫醇霉素中间产物进行羟化。异源宿主的产量提高将能够分离涉及这一令人兴奋的 RiPP 家族生物合成的各个生物合成步骤。

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