Engineering Cytochrome P450BM3 Enzymes for Direct Nitration of Unsaturated Hydrocarbons

Author:

Wang Xiling1,Lin Xiaodan12,Jiang Yiping1,Qin Xiangquan13,Ma Nana12,Yao Fuquan1,Dong Sheng1,Liu Chuanfei1,Feng Yingang1,Jin Longyi3,Xian Mo1,Cong Zhiqi12ORCID

Affiliation:

1. CAS Key Laboratory of Biofuels and Shandong Provincial Key Laboratory of Synthetic Biology Qingdao Institute of Bioenergy and Bioprocess Technology Chinese Academy of Sciences Qingdao Shandong 266101 China

2. University of Chinese Academy of Sciences Beijing 100049 China

3. Department of Chemistry Yanbian University Yanji Jilin 133002 China

Abstract

AbstractApplications of the peroxidase activity of cytochrome P450 enzymes in synthetic chemistry remain largely unexplored. We present herein a protein engineering strategy to increase cytochrome P450BM3 peroxidase activity for the direct nitration of aromatic compounds and terminal aryl‐substituted olefins in the presence of a dual‐functional small molecule (DFSM). Site‐directed mutations of key active‐site residues allowed the efficient regulation of steric effects to limit substrate access and, thus, a significant decrease in monooxygenation activity and increase in peroxidase activity. Nitration of several phenol and aniline compounds also yielded ortho‐ and para‐nitration products with moderate‐to‐high total turnover numbers. Besides direct aromatic nitration by P450 variants using nitrite as a nitrating agent, we also demonstrated the use of the DFSM‐facilitated P450 peroxidase system for the nitration of the vinyl group of styrene and its derivatives.

Funder

Natural Science Foundation of Shandong Province

National Natural Science Foundation of China

Publisher

Wiley

Subject

General Chemistry,Catalysis

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