聚酮合酶
聚酮
阿维菌素
ATP合酶
酶
生物化学
化学
抗生素
开胃菜
生物合成
立体化学
生物
食品科学
解剖
作者
Andrew F. A. Marsden,Barrie Wilkinson,Jesús Cortés,Nicholas J. Dunster,James Staunton,Peter F. Leadlay
出处
期刊:Science
[American Association for the Advancement of Science]
日期:1998-01-09
卷期号:279 (5348): 199-202
被引量:214
标识
DOI:10.1126/science.279.5348.199
摘要
The wide-specificity loading module for the avermectin-producing polyketide synthase was grafted onto the first multienzyme component (DEBS1) of the erythromycin-producing polyketide synthase in place of the normal loading module. Expression of this hybrid enzyme in the erythromycin producer Saccharopolyspora erythraea produced several novel antibiotic erythromycins derived from endogenous branched-chain acid starter units typical of natural avermectins. Because the avermectin polyketide synthase is known to accept more than 40 alternative carboxylic acids as starter units, this approach opens the way to facile production of novel analogs of antibiotic macrolides.
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