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非血红素铁酶催化氧化 C-S 键形成中 S=1 铁(IV)中间产物的揭示

An S=1 Iron(IV) Intermediate Revealed in a Non-Heme Iron Enzyme-Catalyzed Oxidative C-S Bond Formation.

机构信息

Department of Chemistry, Carnegie Mellon University, 4400 Fifth Ave., Pittsburgh, PA 15213, USA.

Department of Chemistry, Boston University, 590 Commonwealth Ave., Boston, MA 02215, USA.

出版信息

Angew Chem Int Ed Engl. 2023 Oct 23;62(43):e202309362. doi: 10.1002/anie.202309362. Epub 2023 Sep 13.

Abstract

Ergothioneine (ESH) and ovothiol A (OSHA) are two natural thiol-histidine derivatives. ESH has been implicated as a longevity vitamin and OSHA inhibits the proliferation of hepatocarcinoma. The key biosynthetic step of ESH and OSHA in the aerobic pathways is the O -dependent C-S bond formation catalyzed by non-heme iron enzymes (e.g., OvoA in ovothiol biosynthesis), but due to the lack of identification of key reactive intermediate the mechanism of this novel reaction is unresolved. In this study, we report the identification and characterization of a kinetically competent S=1 iron(IV) intermediate supported by a four-histidine ligand environment (three from the protein residues and one from the substrate) in enabling C-S bond formation in OvoA from Methyloversatilis thermotoleran, which represents the first experimentally observed intermediate spin iron(IV) species in non-heme iron enzymes. Results reported in this study thus set the stage to further dissect the mechanism of enzymatic oxidative C-S bond formation in the OSHA biosynthesis pathway. They also afford new opportunities to study the structure-function relationship of high-valent iron intermediates supported by a histidine rich ligand environment.

摘要

ergothioneine (ESH) 和 ovothiol A (OSHA) 是两种天然的硫代组氨酸衍生物。ESH 被认为是一种长寿维生素,OSHA 抑制肝癌细胞的增殖。在有氧途径中,ESH 和 OSHA 的关键生物合成步骤是由非血红素铁酶催化的 O-依赖性 C-S 键形成(例如,在 ovothiol 生物合成中 OvoA),但由于关键反应中间体的缺乏,这种新反应的机制尚未解决。在这项研究中,我们报告了在 Methyloversatilis thermotoleran 的 OvoA 中,通过支持 C-S 键形成的四组氨酸配体环境(三个来自蛋白质残基,一个来自底物)鉴定和表征了动力学上有能力的 S=1 铁(IV) 中间产物,这代表了非血红素铁酶中首次观察到的实验中间自旋铁(IV)物种。本研究的结果为进一步剖析 OSHA 生物合成途径中酶促氧化 C-S 键形成的机制奠定了基础。它们还为研究富含组氨酸配体环境支持的高价铁中间体的结构-功能关系提供了新的机会。

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