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Consensus mutagenesis and ancestral reconstruction provide insight into the substrate specificity and evolution of the front-end Δ6-desaturase family

biorxiv. 2020; 
Dongdi Li, Adam M. Damry, James R. Petrie, Thomas Vanhercke, Surinder P. Singh, Colin J. Jackson
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Gene Synthesis The previously constructed pYES2–ura plasmid with the MpΔ6des gene cloned between KpnI and SacI sites was used as the template to generate the desired single mutants. Primer pairs were designed according to the QuikChange site-directed mutagenesis protocol.44 A T7 primer was used with the anti-sense primer and Gal1 terminator primer was used with the sense primer of each mutagenesis primer pair to generate DNA fragments with the desired mutation in the overlapping region. The DNA fragments and the KpnI/SacI-digested pYES2 vector were assembled using an in-house Gibson assembly kit.45 The resulting coding regions were confirmed by sequencing. The 23 algal Δ6 consensus mutants were constructed and cloned by GenScript. Get A Quote

摘要

Marine algae are a major source of omega (ω)-3 long-chain polyunsaturated fatty acids (ω3-LCPUFAs), which are conditionally essential nutrients in humans and a target for industrial production. The biosynthesis of these molecules in marine algae begins with the desaturation of fatty acids by Δ6-desaturases and enzymes from different species display a range of specificities towards ω3 and ω6 LCPUFAs. In the absence of a molecular structure, the structural basis for the variable substrate specificity of Δ6-desaturases is poorly understood. Here we have conducted a consensus mutagenesis and ancestral protein reconstruction-based analysis of the Δ6-desaturase family, focusing on the ω3-specific Δ6-desatura... More

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