Abstract

Existence of homologous proteins that fold into globally different structures signifies an alternative to the concept that structures are more conserved than sequences and demonstrates that protein structures can evolve and change, thus possibly generating new folds and topologies. Our understanding of fold changes in evolution is currently limited to a number of illustrious examples contributed by both experimental studies and computational analysis of available protein structures. Preliminary results demonstrate that structural changes in evolution are more common than is usually accepted. We were able to define four potential mechanisms of fold changes in evolution: insertion deletion/substitution of structural elements, circular permutation, strand invasion, hairpin flip/swap. It is necessary to clarify the scope of these events and to perform a comprehensive analysis of sequence and structure data to find all instances of such changes and classify them. We will undertake comprehensive homology searches for the sequences from proteins families with known structure to find statistically significant sequence similarity links between proteins with different folds. We will analyze the nature of the differences and catalogue possible mechanisms of fold changes in evolution of protein structures. Finally, we will perform in silico evolution of model proteins under functional constraints and compare the results to those deduced from the analysis of natural sequences and structures.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM067165-03
Application #
6936040
Study Section
Molecular and Cellular Biophysics Study Section (BBCA)
Program Officer
Wehrle, Janna P
Project Start
2003-09-01
Project End
2007-08-31
Budget Start
2005-09-01
Budget End
2006-08-31
Support Year
3
Fiscal Year
2005
Total Cost
$280,800
Indirect Cost

  Institution

Name
University of Texas Sw Medical Center Dallas
Department
Biochemistry
Type
Schools of Medicine
DUNS #
800771545
City
Dallas
State
TX
Country
United States
Zip Code
75390

  Publications

Kinch, Lisa N; Li, Wenlin; Monastyrskyy, Bohdan et al. (2016) Assessment of CASP11 contact-assisted predictions. Proteins 84 Suppl 1:164-80
Kinch, Lisa; Yong Shi, Shuo; Cong, Qian et al. (2011) CASP9 assessment of free modeling target predictions. Proteins 79 Suppl 10:59-73
Kinch, Lisa N; Shi, Shuoyong; Cheng, Hua et al. (2011) CASP9 target classification. Proteins 79 Suppl 10:21-36
Pei, Jimin; Grishin, Nick V (2009) The Rho GTPase inactivation domain in Vibrio cholerae MARTX toxin has a circularly permuted papain-like thiol protease fold. Proteins 77:413-9
Pei, Jimin; Ma, Cong; Rizo, Josep et al. (2009) Remote homology between Munc13 MUN domain and vesicle tethering complexes. J Mol Biol 391:509-17
Pei, Jimin; Grishin, Nick V (2009) Prediction of a caspase-like fold in Tannerella forsythia virulence factor PrtH. Cell Cycle 8:1453-5
Wang, Yong; Sadreyev, Ruslan I; Grishin, Nick V (2009) PROCAIN server for remote protein sequence similarity search. Bioinformatics 25:2076-7
Pei, Jimin; Lupardus, Patrick J; Garcia, K Christopher et al. (2009) CPDadh: a new peptidase family homologous to the cysteine protease domain in bacterial MARTX toxins. Protein Sci 18:856-62
Kinch, Lisa N; Yarbrough, Melanie L; Orth, Kim et al. (2009) Fido, a novel AMPylation domain common to fic, doc, and AvrB. PLoS ONE 4:e5818
Sadreyev, Ruslan I; Feramisco, Jamison D; Tsao, Hensin et al. (2009) Phenotypic categorization of genetic skin diseases reveals new relations between phenotypes, genes and pathways. Bioinformatics 25:2891-6

Showing the most recent 10 out of 65 publications