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Creating a more robust 5-hydroxymethylfurfural oxidase by combining computational predictions with a novel effective library design

Biotechnol Biofuels.. 2018-03;  11 (1) :56
Martin C, Ovalle Maqueo A, Wijma HJ, Fraaije MW1. Molecular Enzymology Group, Groningen Biomolecular Sciences and Biotechnology Institute, University of Groningen, Nijenborgh 4, 9747 AG Groningen, The Netherlands
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Gene Synthesis The synthetic genes have been ordered (GenScript) cloned in two pUK57. A derivative of pBAD SUMO vector designed with BsaI cutting site 5′-TGGTngagacc and ggtctcnCTTG-3′) was used as receiving vector. Get A Quote

摘要

Background: HMF oxidase (HMFO) from Methylovorus sp. is a recently characterized flavoprotein oxidase. HMFO is a remarkable enzyme as it is able to oxidize 5-hydroxymethylfurfural (HMF) into 2,5-furandicarboxylic acid (FDCA): a catalytic cascade of three oxidation steps. Because HMF can be formed from fructose or other sugars and FDCA is a polymer building block, this enzyme has gained interest as an industrially relevant biocatalyst. Results: To increase the robustness of HMFO, a requirement for biotechnological applications, we decided to enhance its thermostability using the recently developed FRESCO method: a computational approach to identify thermostabilizing mutations in a protein structure. To make... More

关键词

Carbohydrate; Computational library; Enzyme engineering; Golden Gate gene shuffling; Poly(ethylene-furandicarboxylate) PEF