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PDBsum entry 1vhv

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Transferase PDB id
1vhv
Contents
Protein chains
251 a.a. *
Waters ×363
* Residue conservation analysis

References listed in PDB file
Key reference
Title Structural analysis of a set of proteins resulting from a bacterial genomics project.
Authors J.Badger, J.M.Sauder, J.M.Adams, S.Antonysamy, K.Bain, M.G.Bergseid, S.G.Buchanan, M.D.Buchanan, Y.Batiyenko, J.A.Christopher, S.Emtage, A.Eroshkina, I.Feil, E.B.Furlong, K.S.Gajiwala, X.Gao, D.He, J.Hendle, A.Huber, K.Hoda, P.Kearins, C.Kissinger, B.Laubert, H.A.Lewis, J.Lin, K.Loomis, D.Lorimer, G.Louie, M.Maletic, C.D.Marsh, I.Miller, J.Molinari, H.J.Muller-Dieckmann, J.M.Newman, B.W.Noland, B.Pagarigan, F.Park, T.S.Peat, K.W.Post, S.Radojicic, A.Ramos, R.Romero, M.E.Rutter, W.E.Sanderson, K.D.Schwinn, J.Tresser, J.Winhoven, T.A.Wright, L.Wu, J.Xu, T.J.Harris.
Ref. Proteins, 2005, 60, 787-796. [DOI no: 10.1002/prot.20541]
PubMed id 16021622
Abstract
The targets of the Structural GenomiX (SGX) bacterial genomics project were proteins conserved in multiple prokaryotic organisms with no obvious sequence homolog in the Protein Data Bank of known structures. The outcome of this work was 80 structures, covering 60 unique sequences and 49 different genes. Experimental phase determination from proteins incorporating Se-Met was carried out for 45 structures with most of the remainder solved by molecular replacement using members of the experimentally phased set as search models. An automated tool was developed to deposit these structures in the Protein Data Bank, along with the associated X-ray diffraction data (including refined experimental phases) and experimentally confirmed sequences. BLAST comparisons of the SGX structures with structures that had appeared in the Protein Data Bank over the intervening 3.5 years since the SGX target list had been compiled identified homologs for 49 of the 60 unique sequences represented by the SGX structures. This result indicates that, for bacterial structures that are relatively easy to express, purify, and crystallize, the structural coverage of gene space is proceeding rapidly. More distant sequence-structure relationships between the SGX and PDB structures were investigated using PDB-BLAST and Combinatorial Extension (CE). Only one structure, SufD, has a truly unique topology compared to all folds in the PDB.
Figure 1.
Figure 1. Ribbon diagrams[54] of the eleven structures described in the Results and Discussion section: (A) monomer from the dapE structure (1VGY), (B) homodimer from the nudE structure (1VHG), (C) monomer from the DUS structure (1VHN), (D) monomer from the ysdC structure, 1VHE, (E) monomer from the frwX structure, 1VHO, (F) monomer from the perB structure (1VIZ), (G) monomer from the plsX structure (1VI1), (H) monomer from the yqgF structure (1VHX), (I) monomer from the yigZ structure (1VI7), (J) monomer from the YiiM structure (1O65), (K) the novel sufD structure (1VH4) with the homodimer interface in the center.
The above figure is reprinted by permission from John Wiley & Sons, Inc.: Proteins (2005, 60, 787-796) copyright 2005.
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