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Metabolic engineering of Escherichia coli for the enhanced production of L-tyrosine

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논문

Metabolic engineering of Escherichia coli for the enhanced production of L-tyrosine

학술지

Biotechnology and bioengineering

저자명

Kim, Byoungjin; Binkley, Robert; Kim, Hyun Uk; Lee, Sang Yup

초록

<P>Despite wide applications of L-tyrosine in the market, microbial overproduction of L-tyrosine has been a great challenge due to the complex gene regulations involved in its biosynthetic pathway. To this end, effects of knocking out tyrR on the L-tyrosine production were further explored during the strain development. Also, blocking cellular uptake of L-tyrosine by knocking out tyrosine transporters was examined with respect to L-tyrosine production. Using feedback-resistant aroG and tyrA genes (aroG(fbr) and tyrA(fbr) hereafter) as initial overexpression targets, which encode 3-deoxy-7-phosphoheptulonate synthase and chorismate mutase or prephenate dehydrogenase, respectively, various combinations of genes were subsequently overexpressed in the Escherichia coli wild-type and tyrR knockout strain, and their effects on the L-tyrosine production were examined. Co-overexpression of aroG(fbr), aroL and tyrC, a gene from Zymomonas mobilis functionally similar to tyrA(fbr), but insensitive to L-tyrosine, led to the greatest L-tyrosine production regardless of the strains and plasmid constructs examined in this study. The strain BTY2.13 overexpressing the abovementioned three genes together with the removal of the L-tyrosine-specific transporter (tyrP) produced 43.14g/L of L-tyrosine by fed-batch fermentation using the exponential feeding followed by DO-stat feeding method. This outcome suggested that the tyrR gene knockout was not mandatory for the L-tyrosine overproduction, but the production performance of strains having tyrR appeared to be highly affected by vector systems and feeding methods. With an optimal vector system and a feeding method, tyrP knockout appeared to be more effective in enhancing the L-tyrosine than tyrR knockout.</P>

발행연도

2018

ISSN

0006-3592

ISSN

1097-0290

115

10

페이지

pp.2554-2564

주제어

Escherichia coli; fed&#x2010; batch fermentation; l&#x2010; tyrosine; metabolic engineering;

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1 2023-12-11

논문; 2018-12-31

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