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Rational Design of Flavonoid Production Routes Using Combinatorial and Precursor-Directed Biosynthesis
Author(s) -
Johann E. Kufs,
Sandra Hoefgen,
Julia Rautschek,
Alexander U. Bissell,
Carola Graf,
Jonas Fiedler,
Daniel Braga,
Lars Regestein,
Miriam A. Rosenbaum,
Julian Thiele,
Vito Valiante
Publication year - 2020
Publication title -
acs synthetic biology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.156
H-Index - 66
ISSN - 2161-5063
DOI - 10.1021/acssynbio.0c00172
Subject(s) - synthetic biology , biosynthesis , biochemistry , computational biology , polyketide , metabolic engineering , rational design , enzyme , biology , chemistry , combinatorial chemistry , genetics
Combinatorial biosynthesis has great potential for designing synthetic circuits and amplifying the production of new active compounds. Studies on multienzyme cascades are extremely useful for improving our knowledge on enzymatic catalysis. In particular, the elucidation of enzyme substrate promiscuity can be potentially used for bioretrosynthetic approaches, leading to the design of alternative and more convenient routes to produce relevant molecules. In this perspective, plant-derived polyketides are extremely adaptable to those synthetic biological applications. Here, we present a combination of an in vitro CoA ligase activity assay coupled with a bacterial multigene expression system that leads to precursor-directed biosynthesis of 21 flavonoid derivatives. When the vast knowledge from protein databases is exploited, the herein presented procedure can be easily repeated with additional plant-derived polyketides. Lastly, we report an efficien in vivo expression system that can be further exploited to heterologously express pathways not necessarily related to plant polyketide synthases.

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