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- Title
- Enhanced (-)-alpha-bisabolol productivity by efficient conversion of mevalonate in Escherichia coli = 효율적인 메발로네이트의 전환을 통한 대장균 내 비사볼올 생산성 증대
- Author(s)
- Soo Jung Kim; Seong Keun Kim; Wonjae Seong; Seung Gyun Woo; Hyewon Lee; Soo Jin Yeom; Haseong Kim; Dae-Hee Lee; Seung Goo Lee
- Bibliographic Citation
- Catalysts, vol. 9, pp. 432-432
- Publication Year
- 2019
- Abstract
- (-)-α-Bisabolol, a naturally occurring sesquiterpene alcohol, has been used in
pharmaceuticals and cosmetics owing to its beneficial e ects on inflammation and skin healing.
Previously, we reported the high production of (-)-α-bisabolol by fed-batch fermentation using
engineered Escherichia coli (E. coli) expressing the exogenous mevalonate (MVA) pathway genes.
The productivity of (-)-α -bisabolol must be improved before industrial application. Here, we report
enhancement of initial (-)-α-bisabolol productivity to 3-fold higher than that observed in our previous
study. We first harnessed a farnesyl pyrophosphate (FPP)-resistant mevalonate kinase 1 (MvaK1)
from an archaeon Methanosarcina mazei (M. mazei) to create a more e cient heterologous MVA
pathway that produces (-)-α-bisabolol in the engineered E. coli. The resulting strain produced
1.7-fold higher (-)-α-bisabolol relative to the strain expressing a feedback-inhibitory MvaK1 from
Staphylococcus aureus (S. aureus). Next, to e ciently convert accumulated MVA to (-)-α-bisabolol,
we additionally overexpressed genes involved in the lower MVA mevalonate pathway in E. coli
containing the entire MVA pathway genes. (-)-α-Bisabolol production increased by 1.8-fold with
reduction of MVA accumulation, relative to the control strain. Finally, we optimized the fermentation
conditions including inducer concentration, aeration and enzymatic cofactor. The strain was able to
produce 8.5 g/L of (-)-α-bisabolol with an initial productivity of 0.12 g/L h in the optimal fed-batch
fermentation. Thus, the microbial production of (-)-α-bisabolol would be an economically viable
bioprocess for its industrial application.
- Keyword
- fed-batch fermentationbisabololmevalonate (MVA)mevalonate kinase 1Methanosarcina mazei
- ISSN
- 2073-4344
- Publisher
- MDPI
- Full Text Link
- http://dx.doi.org/10.3390/catal9050432
- Type
- Article
- Appears in Collections:
- Synthetic Biology and Bioengineering Research Institute > Synthetic Biology Research Center > 1. Journal Articles
Korea Biofoundry > 1. Journal Articles
- Files in This Item:
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