Objective: To improve the aroma profile of beer by using metabolic engineering to increase the availability of cytosolic NADH in lager yeast.

Results: To alter NADH levels in lager yeast, the native FDH1 (YOR388C) encoding NAD⁺-dependent formate dehydrogenase was overexpressed in the yeast strain M14, yielding strain M-FDH1. This led to a simultaneous increase of NADH availability and NADH/NAD⁺ ratio in the M-FDH1 strain during fermentation. At the end of the main fermentation period, ethanol production by strain M-FDH1 was decreased by 13.2%, while glycerol production was enhanced by 129.4%, compared to the parental strain respectively. The production of esters and fusel alcohols by strains M14 and M-FDH1 was similar. By contrast, strain M-FDH1 generally produced less organic acids and off-flavor components than strain M14, improving the beer aroma.

Conclusions: Increased NADH availability led to rerouting of the carbon flux toward NADH-consuming pathways and accelerated the NADH-dependent reducing reactions in yeast, greatly impacting the formation of aroma compounds and improving the beer aroma.

• PMID: 30707389
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Journal Article

Authors

Xu X, Bao M, Niu C, Wang J, Liu C, Zheng F, Li Y, Li Q

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