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Biotechnol Bioeng


Title:Continuous cyclohexane oxidation to cyclohexanol using a novel cytochrome P450 monooxygenase from Acidovorax sp. CHX100 in recombinant P. taiwanensis VLB120 biofilms
Author(s):Karande R; Debor L; Salamanca D; Bogdahn F; Engesser KH; Buehler K; Schmid A;
Address:"Department of Solar Materials, Helmholtz-Centre for Environmental Research - UFZ GmbH, Permoserstrasse 15, 04318, Leipzig, Germany. Department of Biochemical and Chemical Engineering, Laboratory of Chemical Biotechnology, TU Dortmund University, Emil-Figge-Strasse 66, 44227, Dortmund, Germany. Department of Biological Waste Air Purification, Institute of Sanitary Engineering, Water Quality and Solid Waste Management, University of Stuttgart, Stuttgart, Germany. Department of Solar Materials, Helmholtz-Centre for Environmental Research - UFZ GmbH, Permoserstrasse 15, 04318, Leipzig, Germany. katja.buehler@ufz.de. Department of Biochemical and Chemical Engineering, Laboratory of Chemical Biotechnology, TU Dortmund University, Emil-Figge-Strasse 66, 44227, Dortmund, Germany. katja.buehler@ufz.de"
Journal Title:Biotechnol Bioeng
Year:2016
Volume:20150918
Issue:1
Page Number:52 - 61
DOI: 10.1002/bit.25696
ISSN/ISBN:1097-0290 (Electronic) 0006-3592 (Linking)
Abstract:"The applications of biocatalysts in chemical industries are characterized by activity, selectivity, and stability. One key strategy to achieve high biocatalytic activity is the identification of novel enzymes with kinetics optimized for organic synthesis by Nature. The isolation of novel cytochrome P450 monooxygenase genes from Acidovorax sp. CHX100 and their functional expression in recombinant Pseudomonas taiwanensis VLB120 enabled efficient oxidation of cyclohexane to cyclohexanol. Although initial resting cell activities of 20 U gCDW (-1) were achieved, the rapid decrease in catalytic activity due to the toxicity of cyclohexane prevented synthetic applications. Cyclohexane toxicity was reduced and cellular activities stabilized over the reaction time by delivering the toxic substrate through the vapor phase and by balancing the aqueous phase mass transfer with the cellular conversion rate. The potential of this novel CYP enzyme was exploited by transferring the shake flask reaction to an aqueous-air segmented flow biofilm membrane reactor for maximizing productivity. Cyclohexane was continuously delivered via the silicone membrane. This ensured lower reactant toxicity and continuous product formation at an average volumetric productivity of 0.4 g L tube (-1) h(-1) for several days. This highlights the potential of combining a powerful catalyst with a beneficial reactor design to overcome critical issues of cyclohexane oxidation to cyclohexanol. It opens new opportunities for biocatalytic transformations of compounds which are toxic, volatile, and have low solubility in water"
Keywords:Biofilms/*growth & development Comamonadaceae/*enzymology/genetics Cyclohexanes/*metabolism/toxicity Cyclohexanols/*metabolism Mixed Function Oxygenases/genetics/*metabolism Oxidation-Reduction Pseudomonas/drug effects/genetics/*metabolism/*physiology Rec;
Notes:"MedlineKarande, Rohan Debor, Linde Salamanca, Diego Bogdahn, Fabian Engesser, Karl-Heinrich Buehler, Katja Schmid, Andreas eng Research Support, Non-U.S. Gov't 2015/07/15 Biotechnol Bioeng. 2016 Jan; 113(1):52-61. doi: 10.1002/bit.25696. Epub 2015 Sep 18"

 
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