Biochemical Characterization of a Flavonoid O -methyltransferase from Perilla Leaves and Its Application in 7-Methoxyflavonoid Production

Methylation is a common structural modification that can alter and improve the biological activities of natural compounds. -Methyltransferases (OMTs) catalyze the methylation of a wide array of secondary metabolites, including flavonoids, and are potentially useful tools for the biotechnological pro...

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Veröffentlicht in:Molecules (Basel, Switzerland) Switzerland), 2020-09, Vol.25 (19), p.4455
Hauptverfasser: Park, Hye Lin, Lee, Jae Chul, Lee, Kyungha, Lee, Jeong Min, Nam, Hyo Jeong, Bhoo, Seong Hee, Lee, Tae Hoon, Lee, Sang-Won, Cho, Man-Ho
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Sprache:eng
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Zusammenfassung:Methylation is a common structural modification that can alter and improve the biological activities of natural compounds. -Methyltransferases (OMTs) catalyze the methylation of a wide array of secondary metabolites, including flavonoids, and are potentially useful tools for the biotechnological production of valuable natural products. An gene ( ) was isolated from perilla leaves as a putative flavonoid OMT (FOMT). Phylogenetic analysis and sequence comparisons showed that PfOMT3 is a class II OMT. Recombinant PfOMT3 catalyzed the methylation of flavonoid substrates, whereas no methylated product was detected in PfOMT3 reactions with phenylpropanoid substrates. Structural analyses of the methylation products revealed that PfOMT3 regiospecifically transfers a methyl group to the 7-OH of flavonoids. These results indicate that PfOMT3 is an FOMT that catalyzes the 7- -methylation of flavonoids. PfOMT3 methylated diverse flavonoids regardless of their backbone structure. Chrysin, naringenin and apigenin were found to be the preferred substrates of PfOMT3. Recombinant PfOMT3 showed moderate OMT activity toward eriodictyol, luteolin and kaempferol. To assess the biotechnological potential of PfOMT3, the biotransformation of flavonoids was performed using -transformed . Naringenin and kaempferol were successfully bioconverted to the 7-methylated products sakuranetin and rhamnocitrin, respectively, by harboring .
ISSN:1420-3049
1420-3049
DOI:10.3390/molecules25194455