Integrated pathway mining and selection of an artificial CYP79-mediated bypass to improve benzylisoquinoline alkaloid biosynthesis

Musashi Takenaka; Kouhei Kamasaka; Kim Daryong; Keiko Tsuchikane; Seiha Miyazawa; Saeko Fujihana; Yoshimi Hori; Christopher J Vavricka; Akira Hosoyama; Hiroko Kawasaki; Tomokazu Shirai; Michihiro Araki; Akira Nakagawa; Hiromichi Minami; Akihiko Kondo; Tomohisa Hasunuma

doi:10.1186/s12934-024-02453-7

Integrated pathway mining and selection of an artificial CYP79-mediated bypass to improve benzylisoquinoline alkaloid biosynthesis

Microb Cell Fact. 2024 Jun 15;23(1):178. doi: 10.1186/s12934-024-02453-7.

Authors

Musashi Takenaka¹, Kouhei Kamasaka², Kim Daryong³, Keiko Tsuchikane³, Seiha Miyazawa³, Saeko Fujihana¹, Yoshimi Hori², Christopher J Vavricka⁴, Akira Hosoyama³, Hiroko Kawasaki³, Tomokazu Shirai⁵, Michihiro Araki^{2

6

7}, Akira Nakagawa⁸, Hiromichi Minami⁸, Akihiko Kondo^{1

2

5

9}, Tomohisa Hasunuma^{10

11

12}

Affiliations

¹ Bacchus Bio innovation Co. Ltd, 6-3-7-505 Minatojima Minamimachi, Chuo-ku, Kobe, 650-0047, Japan.
² Graduate School of Science, Technology and Innovation, Kobe University, 1-1 Rokkodai, Nada, Kobe, 657-8501, Japan.
³ National Institute of Technology and Evaluation, 2-49-10 Nishihara, Shibuya-ku, Tokyo, 1510066, Japan.
⁴ Department of Biotechnology and Life Science, Graduate School of Engineering, Tokyo University of Agriculture and Technology, 2-24-16 Naka-cho, Koganei, Tokyo, 184-8588, Japan.
⁵ Center for Sustainable Resource Science, RIKEN, 1-7-22 Suehiro, Tsurumi, Yokohama, Kanagawa, 230-0045, Japan.
⁶ Graduate School of Medicine, Kyoto University, Yoshida-Konoe-cho, Sakyo-ku, Kyoto, 606- 8501, Japan.
⁷ National Cerebral and Cardiovascular Center, 6-1 Kishibe-Shimmachi, Suita, Osaka, 564-8565, Japan.
⁸ Research Institute for Bioresources and Biotechnology, Ishikawa Prefectural University, 1-308, Suematsu, Nonoichi city, Ishikawa, Japan.
⁹ Engineering Biology Research Center, Kobe University, 1-1 Rokkodai, Nada, Kobe, 657-8501, Japan.
¹⁰ Graduate School of Science, Technology and Innovation, Kobe University, 1-1 Rokkodai, Nada, Kobe, 657-8501, Japan. [email protected].
¹¹ Center for Sustainable Resource Science, RIKEN, 1-7-22 Suehiro, Tsurumi, Yokohama, Kanagawa, 230-0045, Japan. [email protected].
¹² Engineering Biology Research Center, Kobe University, 1-1 Rokkodai, Nada, Kobe, 657-8501, Japan. [email protected].

Abstract

Background: Computational mining of useful enzymes and biosynthesis pathways is a powerful strategy for metabolic engineering. Through systematic exploration of all conceivable combinations of enzyme reactions, including both known compounds and those inferred from the chemical structures of established reactions, we can uncover previously undiscovered enzymatic processes. The application of the novel alternative pathways enables us to improve microbial bioproduction by bypassing or reinforcing metabolic bottlenecks. Benzylisoquinoline alkaloids (BIAs) are a diverse group of plant-derived compounds with important pharmaceutical properties. BIA biosynthesis has developed into a prime example of metabolic engineering and microbial bioproduction. The early bottleneck of BIA production in Escherichia coli consists of 3,4-dihydroxyphenylacetaldehyde (DHPAA) production and conversion to tetrahydropapaveroline (THP). Previous studies have selected monoamine oxidase (MAO) and DHPAA synthase (DHPAAS) to produce DHPAA from dopamine and oxygen; however, both of these enzymes produce toxic hydrogen peroxide as a byproduct.

Results: In the current study, in silico pathway design is applied to relieve the bottleneck of DHPAA production in the synthetic BIA pathway. Specifically, the cytochrome P450 enzyme, tyrosine N-monooxygenase (CYP79), is identified to bypass the established MAO- and DHPAAS-mediated pathways in an alternative arylacetaldoxime route to DHPAA with a peroxide-independent mechanism. The application of this pathway is proposed to result in less formation of toxic byproducts, leading to improved production of reticuline (up to 60 mg/L at the flask scale) when compared with that from the conventional MAO pathway.

Conclusions: This study showed improved reticuline production using the bypass pathway predicted by the M-path computational platform. Reticuline production in E. coli exceeded that of the conventional MAO-mediated pathway. The study provides a clear example of the integration of pathway mining and enzyme design in creating artificial metabolic pathways and suggests further potential applications of this strategy in metabolic engineering.

Keywords: 3,4-dihydroxyphenylacetaldoxime; Artificial metabolic pathway; Benzylisoquinoline alkaloid production; Computational enzyme mining; Cytochrome P450; Tyrosine N-monooxygenase.

MeSH terms

3,4-Dihydroxyphenylacetic Acid / analogs & derivatives
3,4-Dihydroxyphenylacetic Acid / metabolism
Benzylisoquinolines* / metabolism
Biosynthetic Pathways
Computer Simulation
Cytochrome P-450 Enzyme System / metabolism
Escherichia coli* / genetics
Escherichia coli* / metabolism
Metabolic Engineering* / methods
Tetrahydropapaveroline / metabolism

Substances

Benzylisoquinolines
Cytochrome P-450 Enzyme System
Tetrahydropapaveroline
3,4-Dihydroxyphenylacetic Acid