Abstract

WD repeats are ubiquitous 40 amino acids sequence repeats found in hundreds of proteins mediating signal transduction, mRNA splicing, cell cycle regulation, vesicular trafficking, developmental regulation and numerous other physiologically relevant processes involving protein-protein interactions. Accurate modeling and prediction of these proteins' functions demand a complete understanding of how they fold. Based upon the crystal structure of the b subunit of the G protein transducin which has seven repeats and folds into a seven-bladed propeller motif, it has been predicted that the number of blades a particular WD protein has is dictated by the number of WD repeats it possesses, leading to proteins with a variable number of blades. The recent structure of Bub3p, a mitotic checkpoint protein, brings this hypothesis into question. Structures of these proteins will establish a standard model for WD repeat protein structure, one that will be applicable to the hundreds of known sequences as well as the large numbers which will presumably be discovered through ongoing genomic sequencing efforts. In light of the Bub3p structure, a protein believed to contain only four repeats based upon the sequence but found to contain seven in the structure, a hypothesis can be formed that virtually all WD proteins fold into a similar, stable, seven-bladed core structure. Additionally, it also seems likely that these proteins would bind their partner proteins in a similar manner. Preliminary results support this notion. Structural and functional experiments will be conducted to better understand WD repeat proteins and their interactions in general terms 1) the determination of at least four WD protein structures with """"""""irregular"""""""" numbers of repeats predicted by sequence to investigate the possibility of a standard fold and 2) structural, genetic and biochemical characterization of these proteins' interactions with binding partners will determine whether the protein-protein interactions follow a common pattern.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM066135-04
Application #
6915693
Study Section
Biophysical Chemistry Study Section (BBCB)
Program Officer
Flicker, Paula F
Project Start
2002-07-01
Project End
2007-06-30
Budget Start
2005-07-01
Budget End
2007-06-30
Support Year
4
Fiscal Year
2005
Total Cost
$224,385
Indirect Cost

  Institution

Name
University of California Davis
Department
Anatomy/Cell Biology
Type
Schools of Arts and Sciences
DUNS #
047120084
City
Davis
State
CA
Country
United States
Zip Code
95618

  Publications

Di Luccio, Eric; Petschacher, Barbara; Voegtli, Jennifer et al. (2007) Structural and kinetic studies of induced fit in xylulose kinase from Escherichia coli. J Mol Biol 365:783-98
Robins, Lori I; Dixon, Seth M; Wilson, David K et al. (2006) On-bead combinatorial techniques for the identification of selective aldose reductase inhibitors. Bioorg Med Chem 14:7728-35
Di Luccio, Eric; Elling, Robert A; Wilson, David K (2006) Identification of a novel NADH-specific aldo-keto reductase using sequence and structural homologies. Biochem J 400:105-14
Wogulis, Mark; Morgan, Tania; Ishida, Yuko et al. (2006) The crystal structure of an odorant binding protein from Anopheles gambiae: evidence for a common ligand release mechanism. Biochem Biophys Res Commun 339:157-64
Ehrensberger, Andreas H; Elling, Robert A; Wilson, David K (2006) Structure-guided engineering of xylitol dehydrogenase cosubstrate specificity. Structure 14:567-75
Wogulis, Mark; Wheelock, Craig E; Kamita, Shizuo G et al. (2006) Structural studies of a potent insect maturation inhibitor bound to the juvenile hormone esterase of Manduca sexta. Biochemistry 45:4045-57
Wilson, David K; Cerna, David; Chew, Erin (2005) The 1.1-angstrom structure of the spindle checkpoint protein Bub3p reveals functional regions. J Biol Chem 280:13944-51
Leitgeb, Stefan; Petschacher, Barbara; Wilson, David K et al. (2005) Fine tuning of coenzyme specificity in family 2 aldo-keto reductases revealed by crystal structures of the Lys-274-->Arg mutant of Candida tenuis xylose reductase (AKR2B5) bound to NAD+ and NADP+. FEBS Lett 579:763-7
Cerna, David; Wilson, David K (2005) The structure of Sif2p, a WD repeat protein functioning in the SET3 corepressor complex. J Mol Biol 351:923-35
Petschacher, Barbara; Leitgeb, Stefan; Kavanagh, Kathryn L et al. (2005) The coenzyme specificity of Candida tenuis xylose reductase (AKR2B5) explored by site-directed mutagenesis and X-ray crystallography. Biochem J 385:75-83

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