Systems metabolic engineering of Streptomyces venezuelae for the enhanced production of pikromycin

Systems metabolic engineering of Streptomyces venezuelae for the enhanced production of pikromycin

Pikromycin is an important precursor of drugs, for example, erythromycin. Hence, systems metabolic engineering for the enhanced pikromycin production can contribute to the development of pikromycin‐related drugs. In this study, metabolic genes in Streptomyces venezuelae were systematically engineere...

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Veröffentlicht in:Biotechnology and bioengineering 2022-08, Vol.119 (8), p.2250-2260
Hauptverfasser: Cho, Min Kyung, Lee, Byung Tae, Kim, Hyun Uk, Oh, Min‐Kyu
Format: Artikel
Sprache:eng
Schlagworte:
Drug development
Drugs
Erythromycin
Fermentation
gene manipulation targets
Genes
Genomes
genome‐scale metabolic model
Metabolic engineering
Metabolism
Metabolites
Methenyltetrahydrofolate cyclohydrolase
Methylenetetrahydrofolate dehydrogenase
pikromycin
Reductases
Secondary metabolites
Streptomyces venezuelae
Sulfite
Sulfite reductase
Synergistic effect
systems metabolic engineering
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Zusammenfassung:Pikromycin is an important precursor of drugs, for example, erythromycin. Hence, systems metabolic engineering for the enhanced pikromycin production can contribute to the development of pikromycin‐related drugs. In this study, metabolic genes in Streptomyces venezuelae were systematically engineered for enhanced pikromycin production. For this, a genome‐scale metabolic model of S. venezuelae was reconstructed and simulated, which led to the selection of 11 metabolic gene targets. These metabolic genes, including four overexpression targets and seven knockdown targets, were individually engineered first. Next, two overexpression targets and two knockdown targets were selected based on the 11 strains' production performances to engineer two to four of these genes together for the potential synergistic effects on the pikromycin production. As a result, the NM1 strain with AQF52_RS24510 (methenyltetrahydrofolate cyclohydrolase/methylenetetrahydrofolate dehydrogenase) overexpression and AQF52_RS30320 (sulfite reductase) knockdown showed the best production performance among all the 22 strains constructed in this study. Fed‐batch fermentation of the NM1 strain produced 295.25 mg/L of pikromycin, by far the best production titer using the native producer S. venezuelae, to the best of our knowledge. The systems metabolic engineering strategy demonstrated herein can also be applied to the overproduction of other secondary metabolites using S. venezuelae. Pikromycin is an important precursor of drugs, including antibiotics and anticancers. Hence, systems metabolic engineering for the enhanced pikromycin production can contribute to the development of pikromycin‐related drugs. In this study, metabolic genes in Streptomyces venezuelae were systematically engineered by using a genome‐scale metabolic model for enhanced pikromycin production. Fed‐batch fermentation of the final engineered strain produced 295.25 mg/L of pikromycin, by far the best production titer using the native producer S. venezuelae.
ISSN:0006-3592
1097-0290
DOI:10.1002/bit.28114