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环己酮单加氧酶的内酯结合结构有助于深入了解催化反应的立体化学。

Lactone-bound structures of cyclohexanone monooxygenase provide insight into the stereochemistry of catalysis.

作者信息

Yachnin Brahm J, McEvoy Michelle B, MacCuish Roderick J D, Morley Krista L, Lau Peter C K, Berghuis Albert M

机构信息

Departments of †Biochemistry and ‡Microbiology & Immunology, McGill University , 3649 Promenade Sir William Osler, Bellini Pavilion, Room 466, Montreal, Quebec, Canada H3G 0B1.

出版信息

ACS Chem Biol. 2014 Dec 19;9(12):2843-51. doi: 10.1021/cb500442e. Epub 2014 Oct 21.

Abstract

The Baeyer-Villiger monooxygenases (BVMOs) are microbial enzymes that catalyze the synthetically useful Baeyer-Villiger oxidation reaction. The available BVMO crystal structures all lack a substrate or product bound in a position that would determine the substrate specificity and stereospecificity of the enzyme. Here, we report two crystal structures of cyclohexanone monooxygenase (CHMO) with its product, ε-caprolactone, bound: the CHMO(Tight) and CHMO(Loose) structures. The CHMO(Tight) structure represents the enzyme state in which substrate acceptance and stereospecificity is determined, providing a foundation for engineering BVMOs with altered substrate spectra and/or stereospecificity. The CHMO(Loose) structure is the first structure where the product is solvent accessible. This structure represents the enzyme state upon binding and release of the substrate and product. In addition, the role of the invariant Arg329 in chaperoning the substrate/product during the catalytic cycle is highlighted. Overall, these data provide a structural framework for the engineering of BVMOs with altered substrate spectra and/or stereospecificity.

摘要

拜耳-维利格单加氧酶(BVMOs)是一类催化具有合成价值的拜耳-维利格氧化反应的微生物酶。现有的BVMO晶体结构均未在能决定酶的底物特异性和立体特异性的位置结合底物或产物。在此,我们报道了环己酮单加氧酶(CHMO)与其产物ε-己内酯结合的两种晶体结构:CHMO(紧密型)和CHMO(松散型)结构。CHMO(紧密型)结构代表了决定底物接纳和立体特异性的酶状态,为改造具有改变的底物谱和/或立体特异性的BVMOs奠定了基础。CHMO(松散型)结构是产物可被溶剂接触的首个结构。该结构代表了底物和产物结合及释放后的酶状态。此外,还突出了保守的Arg329在催化循环中陪伴底物/产物的作用。总体而言,这些数据为改造具有改变的底物谱和/或立体特异性的BVMOs提供了结构框架。

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