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一种类血红素加氧酶切除次甲基的结构基础。

Structural Basis for Methine Excision by a Heme Oxygenase-like Enzyme.

作者信息

Simke William C, Walker Morgan E, Calderone Logan A, Putz Andrew T, Patteson Jon B, Vitro Caitlin N, Zizola Cynthia F, Redinbo Matthew R, Pandelia Maria-Eirini, Grove Tyler L, Li Bo

机构信息

Department of Chemistry, The University of North Carolina at Chapel Hill, Chapel Hill, North Carolina 27599, United States.

Department of Biochemistry, Brandeis University, 415 South Street, Waltham, Massachusetts 02453, United States.

出版信息

ACS Cent Sci. 2024 Jul 24;10(8):1524-1536. doi: 10.1021/acscentsci.4c00015. eCollection 2024 Aug 28.

Abstract

Heme oxygenase-like domain-containing oxidases (HDOs) are a rapidly expanding enzyme family that typically use dinuclear metal cofactors instead of heme. FlcD, an HDO from the opportunistic pathogen , catalyzes the excision of an oxime carbon in the biosynthesis of the copper-containing antibiotic fluopsin C. We show that FlcD is a dioxygenase that catalyzes a four-electron oxidation. Crystal structures of FlcD reveal a mononuclear iron in the active site, which is coordinated by two histidines, one glutamate, and the oxime of the substrate. Enzyme activity, Mössbauer spectroscopy, and electron paramagnetic resonance spectroscopy analyses support the usage of a mononuclear iron cofactor. This cofactor resembles that of mononuclear non-heme iron-dependent enzymes and breaks the paradigm of dinuclear HDO cofactors. This study begins to illuminate the catalytic mechanism of methine excision and indicates convergent evolution of different lineages of mononuclear iron-dependent enzymes.

摘要

含血红素加氧酶样结构域的氧化酶(HDOs)是一个迅速扩展的酶家族,其通常使用双核金属辅因子而非血红素。FlcD是一种来自机会致病菌的HDO,在含铜抗生素氟视紫红质C的生物合成中催化肟碳的切除。我们发现FlcD是一种催化四电子氧化的双加氧酶。FlcD的晶体结构显示活性位点中有一个单核铁,它由两个组氨酸、一个谷氨酸和底物的肟配位。酶活性、穆斯堡尔光谱和电子顺磁共振光谱分析支持单核铁辅因子的使用。这种辅因子类似于单核非血红素铁依赖性酶的辅因子,打破了双核HDO辅因子的模式。这项研究开始阐明次甲基切除的催化机制,并表明单核铁依赖性酶不同谱系的趋同进化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5bdf/11363339/34b1d90fa005/oc4c00015_0001.jpg

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