放线菌门
生物合成
酶
化学
甲基转移酶
萜烯
生物化学
立体化学
甲基化
生物
基因
16S核糖体RNA
作者
Tatjana Reuter,Lars Dieminger,Sarah Steidle,Katrin Zoller,Maximilian Holocher,Lin Zhou,Dominik Hanauska,Károly Rácz,Lena Barra
标识
DOI:10.1002/anie.202418613
摘要
A novel biosynthetic pathway towards the rare and underexplored non‐canonical family of homoterpenes was discovered in actinobacteria through targeted genome mining and enzymatic in vitro reconstitution. The pathway comprises initial methylation‐induced double bond isomerization of farnesyl diphosphate (FPP) to (2E,7E)‐6‐methyl‐farnesyl diphosphate, catalyzed by a novel family of methyltransferases with unique dual function. The resulting linear C16 double bond isomer of FPP constitutes the specific substrate for a distinct family of type I terpene cyclases, catalyzing diverse cyclization reactions. Functional characterization of nine enzyme pairs led to discovery of five unprecedented homoterpene natural products. The enzymological novelty enable the development of novel biocatalytic and genetically programmable synthetic strategies towards methylated terpenoids with potentially unique properties (“magic methyl effect”).
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