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Optimization of a heterologous mevalonate pathway through the use of variant HMG-CoA reductases.

Metab Eng.. 2011-09;  13(5):588-97
Ma SM, Garcia DE, Redding-Johanson AM, Friedland GD, Chan R, Batth TS, Haliburton JR, Chivian D, Keasling JD, Petzold CJ, Lee TS, Chhabra SR. a Joint BioEnergy Institute, Emeryville, CA, United Statesb Physical Biosciences Division, Lawrence Berkeley National Laboratory, Berkeley, CA, United Statesc Departments of Chemical Engineering and Bioengineering, University of California, Berkeley, CA, United Statesd Biomass Science and Conversion Technology Department, Sandia National Laboratories, Livermore, CA, United Statese Department of Chemistry, University of California, Berkeley, CA, United States
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摘要

Expression of foreign pathways often results in suboptimal performance due to unintended factors such as introduction of toxic metabolites, cofactor imbalances or poor expression of pathway components. In this study we report a 120% improvement in the production of the isoprenoid-derived sesquiterpene, amorphadiene, produced by an engineered strain of Escherichia coli developed to express the native seven-gene mevalonate pathway from Saccharomyces cerevisiae (Martin et al. 2003). This substantial improvement was made by varying only a single component of the pathway (HMG-CoA reductase) and subsequent host optimization to improve cofactor availability. We characterized and tested five variant HMG-CoA reductases ... More

关键词

Mevalonate pathway; Metabolic pathway optimization; HMG-CoA Reductase; E. coli; Cofactor regeneration; Mevalonate kinase