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Repression of mitochondrial metabolism for cytosolic pyruvate-derived chemical production in Saccharomyces cerevisiae

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논문

Repression of mitochondrial metabolism for cytosolic pyruvate-derived chemical production in Saccharomyces cerevisiae

학술지

Microbial cell factories

저자명

Morita, Keisuke; Matsuda, Fumio; Okamoto, Koji; Ishii, Jun; Kondo, Akihiko; Shimizu, Hiroshi

초록

<B>Abstract</B><B>Background</B><P><I>Saccharomyces cerevisiae</I> is a suitable host for the industrial production of pyruvate-derived chemicals such as ethanol and 2,3-butanediol (23BD). For the improvement of the productivity of these chemicals, it is essential to suppress the unnecessary pyruvate consumption in <I>S. cerevisiae</I> to redirect the metabolic flux toward the target chemical production. In this study, mitochondrial pyruvate transporter gene (<I>MPC1</I>) or the essential gene for mitophagy (<I>ATG32</I>) was knocked-out to repress the mitochondrial metabolism and improve the production of pyruvate-derived chemical in <I>S. cerevisiae</I>.</P><B>Results</B><P>The growth rates of both aforementioned strains were 1.6-fold higher than that of the control strain. <SUP>13</SUP>C-metabolic flux analysis revealed that both strains presented similar flux distributions and successfully decreased the tricarboxylic acid cycle fluxes by 50% compared to the control strain. Nevertheless, the intracellular metabolite pool sizes were completely different, suggesting distinct metabolic effects of gene knockouts in both strains. This difference was also observed in the test-tube culture for 23BD production. Knockout of <I>ATG32</I> revealed a 23.6-fold increase in 23BD titer (557.0 ± 20.6 mg/L) compared to the control strain (23.5 ± 12.8 mg/L), whereas the knockout of <I>MPC1</I> revealed only 14.3-fold increase (336.4 ± 113.5 mg/L). Further investigation using the anaerobic high-density fermentation test revealed that the <I>MPC1</I> knockout was more effective for ethanol production than the 23BD production.</P><B>Conclusion</B><P>These results suggest that the engineering of the mitochondrial transporters and membrane dynamics were effective in controlling the mitochondrial metabolism to improve the productivities of chemicals in yeast cytosol.</P>

발행연도

2019

발행기관

Springer (Biomed Central Ltd.)

라이선스

cc-by

ISSN

1475-2859

18

페이지

pp.177

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1 2023-12-11
2 2023-12-11

논문; 2019-10-15

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