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来自罗尔斯通氏菌的一种拜耳-维利格单加氧酶催化(R)-兰索拉唑和其他药物亚砜的不对称合成。

A Baeyer-Villiger monooxygenase from Cupriavidus basilensis catalyzes asymmetric synthesis of (R)-lansoprazole and other pharmaco-sulfoxides.

作者信息

Liu Feng, Shou Chao, Geng Qiang, Zhao Chen, Xu Jianhe, Yu Huilei

机构信息

State Key Laboratory of Bioreactor Engineering, Shanghai Collaborative Innovation Center for Biomanufacturing and School of Biotechnology, East China University of Science and Technology, 130 Meilong Road, Shanghai, 200237, China.

出版信息

Appl Microbiol Biotechnol. 2021 Apr;105(8):3169-3180. doi: 10.1007/s00253-021-11230-0. Epub 2021 Mar 29.

Abstract

Biocatalytic synthesis of pharmaco-chiral sulfoxides has gained interest in recent years for its environmental friendliness. However, only a few natural biocatalysts can be used for the efficient synthesis of pharmaco-sulfoxides, including (R)-lansoprazole, a chiral proton pump inhibitor used to treat gastrointestinal diseases. In this study, the sequence of BoBVMO (Baeyer-Villiger monooxygenase from Bradyrhizobium oligotrophicum) was used as a probe to identify BVMOs via genomic mining for the highly efficient synthesis of (R)-lansoprazole and other pharmaco-sulfoxides. After virtual sequence filtering, target gene cloning, heterologous expression, and activity screening for lansoprazole sulfide (LPS) monooxygenation, seven new BVMOs were identified among more than 10,000 homologous BVMOs. According to the conserved sequence and phylogenetic tree analysis, these discovered enzymes belong to the family of type I BVMOs and the ethionamide monooxygenase subtype. Among them, CbBVMO, Baeyer-Villiger monooxygenase from Cupriavidus basilensis, showed the highest efficiency and excellent enantioselectivity for converting LPS into (R)-lansoprazole. Moreover, CbBVMO showed a wide substrate spectrum toward other bulky prazole-family sulfides. The results indicate that CbBVMO is a potential enzyme for extending the application of BVMOs in pharmaceutical industry. KEY POINTS: • CbBVMO is the most efficient biocatalyst for (R)-lansoprazole biosynthesis. • CbBVMO catalyzes the conversion of various bulky prazole sulfides. • CbBVMO is a promising enzyme for the biosynthesis of pharmaco-sulfoxides.

摘要

近年来,生物催化合成药物手性亚砜因其环境友好性而备受关注。然而,只有少数天然生物催化剂可用于高效合成药物亚砜,包括(R)-兰索拉唑,一种用于治疗胃肠道疾病的手性质子泵抑制剂。在本研究中,以寡营养慢生根瘤菌的Baeyer-Villiger单加氧酶(BoBVMO)序列为探针,通过基因组挖掘来鉴定用于高效合成(R)-兰索拉唑和其他药物亚砜的单加氧酶(BVMO)。经过虚拟序列筛选、目标基因克隆、异源表达以及对兰索拉唑硫化物(LPS)单加氧反应的活性筛选后,在10000多个同源BVMO中鉴定出7种新的BVMO。根据保守序列和系统发育树分析,这些发现的酶属于I型BVMO家族和乙硫异烟胺单加氧酶亚型。其中,来自罗尔斯通氏菌的Baeyer-Villiger单加氧酶(CbBVMO)在将LPS转化为(R)-兰索拉唑方面表现出最高效率和出色的对映选择性。此外,CbBVMO对其他大分子的拉唑类硫化物显示出广泛的底物谱。结果表明,CbBVMO是一种有潜力的酶,可扩展BVMO在制药工业中的应用。要点:•CbBVMO是(R)-兰索拉唑生物合成中最有效的生物催化剂。•CbBVMO催化各种大分子拉唑硫化物的转化。•CbBVMO是一种有前途的用于药物亚砜生物合成的酶。

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