Enantioselective, continuous (R)- and (S)-2-butanol synthesis: Achieving high space-time yields with recombinant E. coli cells in a micro-aqueous, solvent-free reaction system

Enantioselective, continuous (R)- and (S)-2-butanol synthesis: Achieving high space-time yields with recombinant E. coli cells in a micro-aqueous, solvent-free reaction system

•Biocatalytic, stereoselective 2-butanone reduction in continuous micro-aqueous system.•High conversions (>95%) and ee (>96%) achieved for (R)-2-butanol.•Extremely high space-time yields were obtained.•System was successfully transferred to a (S)-selective catalyst. The stereoselective product...

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Bibliographic Details
Published in:Journal of biotechnology Vol. 191; pp. 106 - 112
Main Authors: Erdmann, Vanessa, Mackfeld, Ursula, Rother, Dörte, Jakoblinnert, Andre
Format: Journal Article
Language:English
Published: Netherlands Elsevier B.V 10-12-2014
Subjects:
2-Butanol
Alcohol dehydrogenase
Alcohol Dehydrogenase - chemistry
Alcohol Dehydrogenase - genetics
Asymmetry
Biocatalysis
Biotechnology
Butanols - chemical synthesis
Butanols - chemistry
Butanones - chemistry
Continuous system
Conversion
Escherichia coli
Escherichia coli - enzymology
Escherichia coli - genetics
Lactobacillus brevis
Lactobacillus brevis - enzymology
Lactobacillus brevis - genetics
Micro-aqueous
Racemisation
Recombinant
Recombinant Proteins
Stereoisomerism
Stereoselectivity
Strategy
Substrate Specificity
Synthesis
RT
CPCR
τ
ADH
MSTFA
NADP+/NADPH
R
S
2-Butanol
Lb
pH
STY
v/v
GC
E. coli
ee
Racemisation
c
PTFE
HCD
CMR
rpm
TB
TEA
LbADH
MeOH
Micro-aqueous
Continuous system
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Summary:•Biocatalytic, stereoselective 2-butanone reduction in continuous micro-aqueous system.•High conversions (>95%) and ee (>96%) achieved for (R)-2-butanol.•Extremely high space-time yields were obtained.•System was successfully transferred to a (S)-selective catalyst. The stereoselective production of (R)- or (S)-2-butanol is highly challenging. A potent synthesis strategy is the biocatalytic asymmetric reduction of 2-butanone applying alcohol dehydrogenases. However, due to a time-dependent racemisation process, high stereoselectivity is only obtained at incomplete conversion after short reaction times. Here, we present a solution to this problem: by using a continuous process, high biocatalytic selectivity can be achieved while racemisation is suppressed successfully. Furthermore, high conversion was achieved by applying recombinant, lyophilised E. coli cells hosting Lactobacillus brevis alcohol dehydrogenase in a micro-aqueous solvent-free continuous reaction system. The optimisation of residence time (τ) and 2-butanone concentration boosted both conversion (>99%) and enantiomeric excess (ee) of (R)-2-butanol (>96%). When a residence time of only τ=3.1 min was applied, productivity was extraordinary with a space-time yield of 2278±29g/(L×d), thus exceeding the highest values reported to date by a factor of more than eight. The use of E. coli cells overexpressing an ADH of complementary stereoselectivity yielded a synthesis strategy for (S)-2-butanol with an excellent ee (>98%). Although conversion was only moderate (up to 46%), excellent space-time yields of up to 461g/(L×d) were achieved. The investigated concept represents a synthesis strategy that can also be applied to other biocatalytic processes where racemisation poses a challenge.
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ISSN:0168-1656
1873-4863
DOI:10.1016/j.jbiotec.2014.06.032