
A repeating theme in the structural biology of disulfide oxidants and isomerases is the extraordinary architectural similarity between functionally related proteins from prokaryotes and eukaryotes. The recently determined structure of full-length yeast protein disulfide isomerase (PDI) reveals a U-shaped molecule with two redox-active sites. It bears a remarkable resemblance to the V-shaped, but dimeric, bacterial disulfide isomerases DsbC and DsbG. Similarly, the much-anticipated structure of the bacterial membrane protein DsbB, the redox partner of DsbA, comprises a flexible redox loop embedded in an antiparallel four-helix bundle. This architecture is similar to that of soluble eukaryotic Ero1p and Erv2p proteins, the redox partners of PDI. Importantly, the DsbB crystal structure is a complex with DsbA, providing our first view of the molecular interactions between these two proteins.
Models, Molecular, 780105 Biological sciences, Biochemistry and cell biology not elsewhere classified, remarkable resemblance, Proteins, pdi, 612, protein disulfide isomerase, proteins, Redox, 270199 Biochemistry and Cell Biology not elsewhere classified, C1, yeast protein, Biochemistry and cell biology, Medicinal and biomolecular chemistry, membrane protein, s r Martin, Disulfides, prokaryotes and eukaryotes, Oxidation-Reduction, disulfide
Models, Molecular, 780105 Biological sciences, Biochemistry and cell biology not elsewhere classified, remarkable resemblance, Proteins, pdi, 612, protein disulfide isomerase, proteins, Redox, 270199 Biochemistry and Cell Biology not elsewhere classified, C1, yeast protein, Biochemistry and cell biology, Medicinal and biomolecular chemistry, membrane protein, s r Martin, Disulfides, prokaryotes and eukaryotes, Oxidation-Reduction, disulfide
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