代谢工程
效价
代谢途径
突变体
基因
计算生物学
合成生物学
生物
生物技术
生物化学
遗传学
抗体
作者
J. Andrew Jones,Victoria R. Vernacchio,Daniel M. Lachance,Matthew Lebovich,Li Fu,Abhijit N. Shirke,Victor Schultz,Brady F. Cress,Robert J. Linhardt,Mattheos A. G. Koffas
摘要
The ability to fine tune gene expression has created the field of metabolic pathway optimization and balancing where a variety of factors affecting flux balance are carefully modulated to improve product titers, yields, and productivity. Using a library of isopropyl β-D-1-thiogalactopyranoside (IPTG)-inducible mutant T7 promoters of varied strength a combinatorial method was developed for transcriptional balancing of the violacein pathway. Violacein biosynthesis involves a complex five-gene pathway that is an excellent model for exploratory metabolic engineering efforts into pathway regulation and control due to many colorful intermediates and side products allowing for easy analysis and strain comparison. Upon screening approximately 4% of the total initial library, several high-titer mutants were discovered that resulted in up to a 63-fold improvement over the control strain. With further fermentation optimization, titers were improved to 1829 ± 46 mg/L; a 2.6-fold improvement in titer and a 30-fold improvement in productivity from previous literature reports.
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