Identification of biosynthetic genes for the β-carboline alkaloid kitasetaline and production of the fluorinated derivatives by heterologous expression

Author:

Ueda Shohei1,Ikeda Haruo2,Namba Takushi3,Ikejiri Yukinori1,Nishimoto Yuri1,Arai Masayoshi4,Nihira Takuya15,Kitani Shigeru1

Affiliation:

1. 0000 0004 0373 3971 grid.136593.b International Center for Biotechnology Osaka University 2-1 Yamadaoka 565-0871 Suita Osaka Japan

2. 0000 0000 9206 2938 grid.410786.c Kitasato Institute for Life Sciences Kitasato University 1-15-1 Kitasato 252-0373 Sagamihara Kanagawa Japan

3. 0000 0001 0659 9825 grid.278276.e Science Research Center Kochi University Kohasu, Oko-cho 783-8505 Nankoku Kochi Japan

4. 0000 0004 0373 3971 grid.136593.b Graduate School of Pharmaceutical Sciences Osaka University 1-6 Yamadaoka 565-0871 Suita Osaka Japan

5. 0000 0004 1937 0490 grid.10223.32 MU-OU Collaborative Research Center for Bioscience and Biotechnology, Faculty of Science Mahidol University Rama VI Rd 10400 Bangkok Thailand

Abstract

Abstract β-Carboline alkaloids exhibit a broad spectrum of pharmacological and biological activities and are widely distributed in nature. Genetic information on the biosynthetic mechanism of β-carboline alkaloids has not been accumulated in bacteria, because there are only a few reports on the microbial β-carboline compounds. We previously isolated kitasetaline, a mercapturic acid derivative of a β-carboline compound, from the genetically modified Kitasatospora setae strain and found a plausible biosynthetic gene cluster for kitasetaline. Here, we identified and characterized three kitasetaline (ksl) biosynthetic genes for the formation of the β-carboline core structure and a gene encoding mycothiol-S-conjugate amidase for the modification of the N-acetylcysteine moiety by using heterologous expression. The proposed model of kitasetaline biosynthesis shows unique enzymatic systems for β-carboline alkaloids. In addition, feeding fluorotryptophan to the heterologous Streptomyces hosts expressing the ksl genes led to the generation of unnatural β-carboline alkaloids exerting novel/potentiated bioactivities.

Funder

Japan Society for the Promotion of Science

The Japan Association for Chemical Innovation

Publisher

Oxford University Press (OUP)

Subject

Applied Microbiology and Biotechnology,Biotechnology,Bioengineering

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