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Structural and biochemical analyses reveal insights into covalent flavinylation of the Complex II homolog quinol:fumarate reductase

J Biol Chem. 2017-06-01; 
C A Starbird, Elena Maklashina, Pankaj Sharma, Susan Qualls-Histed, Gary Cecchini, T M Iverson
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PCR Cloning and Subcloning … 31190) and pEVOL-pAzF (catalog no. 31186) vectors were obtained from Addgene (Cambridge, MA). To create pQE-SdhE, the E. coli ygfYX operon was synthesized (GenScript) with a 5′ BamHI site and a 3′ SalI site to facilitate cloning into the pQE-80L (Qiagen) vector … Get A Quote

摘要

The Complex II homolog quinol:fumarate reductase (QFR, FrdABCD) catalyzes the interconversion of fumarate and succinate at a covalently attached FAD within the FrdA subunit. The SdhE assembly factor enhances covalent flavinylation of Complex II homologs, but the mechanisms underlying the covalent attachment of FAD remain to be fully elucidated. Here, we explored the mechanisms of covalent flavinylation of the QFR FrdA subunit. Using a Δ strain, we show that the requirement for the assembly factor depends on the cellular redox environment. We next identified residues important for the covalent attachment and selected the FrdA residue, which contributes to proton shuttling during fumarate reduction, for detail... More

关键词

Complex II, bioenergetics, flavin adenine dinucleotide (FAD), membrane enzyme, oxidation-reduction (redox), protein assembly, protein structure, respiratory chain