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In vitro reconstitution of mevalonate pathway and targeted engineering of farnesene overproduction in Escherichia coli

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논문

In vitro reconstitution of mevalonate pathway and targeted engineering of farnesene overproduction in Escherichia coli

학술지

Biotechnology and bioengineering

저자명

Zhu, Fayin; Zhong, Xiaofang; Hu, Mengzhu; Lu, Lei; Deng, Zixin; Liu, Tiangang

초록

<P><B>ABSTRACT</B></P><P>Approaches using metabolic engineering and synthetic biology to overproduce terpenoids, such as the precursors of taxol and artemisinin, in microbial systems have achieved initial success. However, due to the lack of steady&#8208;state kinetic information and incomplete understanding of the terpenoid biosynthetic pathway, it has been difficult to build a highly efficient, universal system. Here, we reconstituted the mevalonate pathway to produce farnesene (a precursor of new jet fuel) in vitro using purified protein components. The information from this in vitro reconstituted system guided us to rationally optimize farnesene production in <I>E. coli</I> by quantitatively overexpressing each component. Targeted proteomic assays and intermediate assays were used to determine the metabolic status of each mutant. Through targeted engineering, farnesene production could be increased predictably step by step, up to 1.1&thinsp;g/L (&sim;2,000 fold) 96&thinsp;h after induction at the shake&#8208;flask scale. The strategy developed to release the potential of the mevalonate pathway for terpenoid overproduction should also work in other multistep synthetic pathways. Biotechnol. Bioeng. 2014;111: 1396&ndash;1405. &copy; 2014 Wiley Periodicals, Inc.</P>

발행연도

2014

ISSN

0006-3592

ISSN

1097-0290

111

7

페이지

pp.1396-1405

주제어

mevalonate pathway; in vitro reconstitution; terpenoid; farnesene; targeted engineering; biofuel

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논문; 2014-12-31

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