Chemoenzymatic Synthesis of 2‐Aryl Thiazolines from 4‐Hydroxybenzaldehydes Using Vanillyl Alcohol Oxidases

Author:

Zhang Haowen1,Xie Shuhan2,Yang Jun13,Ye Ning45,Gao Feng4,Gallou Fabrice6,Gao Lei1ORCID,Lei Xiaoguang13ORCID

Affiliation:

1. Beijing National Laboratory for Molecular Sciences Key Laboratory of Bioorganic Chemistry and Molecular Engineering of Ministry of Education College of Chemistry and Molecular Engineering Peking University Beijing 100871 People's Republic of China

2. Department of Biological Sciences Xi'an Jiaotong-Liverpool University Suzhou 215123 People's Republic of China

3. Peking-Tsinghua Center for Life Science Academy for Advanced Interdisciplinary Studies Peking University Beijing 100871 People's Republic of China

4. Chemical & Analytical Development Suzhou Novartis Technical Development Co., Ltd. Changshu 215537 People's Republic of China

5. Current Address: Rezubio Pharmaceuticals Co., Ltd. Zhuhai 519070 People's Republic of China

6. Chemical and Analytical Development, Novartis Pharma AG, Novartis Campus Basel 4056 Switzerland

Abstract

AbstractNitrogen heterocycles are commonly found in bioactive natural products and drugs. However, the biocatalytic tools for nitrogen heterocycle synthesis are limited. Herein, we report the discovery of vanillyl alcohol oxidases (VAOs) as efficient biocatalysts for the one‐pot synthesis of 2‐aryl thiazolines from various 4‐hydroxybenzaldehydes and aminothiols. The wild‐type biocatalyst features a broad scope of 4‐hydroxybenzaldehydes. Though the scope of aminothiols is limited, it could be improved via semi‐rational protein engineering, generating a variant to produce previously inaccessible cysteine‐derived bioactive 2‐aryl thiazolines using the wild‐type VAO. Benefiting from the derivatizable functional groups in the enzymatic products, we further chemically modified these products to expand the chemical space, offering a new chemoenzymatic strategy for the green and efficient synthesis of structurally diverse 2‐aryl‐thiazoline derivatives to prompt their use in drug discovery and catalysis.

Publisher

Wiley

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