Abstract

In this project we will develop a computational approach to model membrane proteins for which a limited number of experimental restraints are available but for which the experimental structure is difficult to obtain. We will utilize our recently developed fragment library of supersecondary structure elements (Smotifs) that exhaustively classifies all known building blocks of proteins. Recently we have shown that this library of Smotifs saturated almost 10 years ago, and that new folds seem to be a novel combination of existing Smotifs. Therefore we hypothesize that all protein folds should be possible to build from this library. In order to model membrane proteins we can calculate hypothetical chemical shift values for all our Smotifs, while chemical shift values for a protein of interest can usually be quickly and easily obtained and assigned from initial NMR experiments. This proposal is concerned with developing algorithms that can match experimentally observed and theoretically calculated chemical shift patterns of Smotifs and therefore identify a subset of Smotif conformations that form a protein. The second part of the proposal is concerned of setting up an optimization approach (a sampling algorithm along the degrees of freedom of Smotif combinations and a scoring function) that will rapidly assemble overlapping Smotifs into compact folds using additional experimental restraints obtained from NMR dipolar coupling data. In later years of the project we will apply our technique on specific proteins for which chemical shift and dipolar coupling data were obtained and subsequently verify our computational models with spin labeling experiments. The technologies developed in this application will provide the foundation required for efficient modeling of membrane proteins for which a very limited number of experimental structures are available in the PDB. Meanwhile membrane proteins constitute the majority of targets of currently known drugs. Our effort is focused on increasing the rate of discovering membrane protein structures and therefore will lay a foundation for more effective rational drug design.

Public Health Relevance

The majority of currently known drugs target membrane proteins, of which only about 0.5% have been structurally characterized. In this proposal we will develop a fragment assembly modeling approach that takes advantage of NMR chemical shift data and our recently developed supersecondary structure library. Our effort is concerned with increasing the rate of discovering membrane protein structures and will lay a foundation for effective rational drug design for this important class of proteins.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM096041-01
Application #
8025220
Study Section
Macromolecular Structure and Function D Study Section (MSFD)
Program Officer
Smith, Ward
Project Start
2011-05-01
Project End
2015-04-30
Budget Start
2011-05-01
Budget End
2012-04-30
Support Year
1
Fiscal Year
2011
Total Cost
$315,400
Indirect Cost

  Institution

Name
Albert Einstein College of Medicine
Department
Biology
Type
Schools of Medicine
DUNS #
110521739
City
Bronx
State
NY
Country
United States
Zip Code
10461

  Publications

Dybas, Joseph M; Fiser, Andras (2016) Development of a motif-based topology-independent structure comparison method to identify evolutionarily related folds. Proteins 84:1859-1874
Vallat, Brinda; Madrid-Aliste, Carlos; Fiser, Andras (2015) Modularity of Protein Folds as a Tool for Template-Free Modeling of Structures. PLoS Comput Biol 11:e1004419
Pujato, Mario; Kieken, Fabien; Skiles, Amanda A et al. (2014) Prediction of DNA binding motifs from 3D models of transcription factors; identifying TLX3 regulated genes. Nucleic Acids Res 42:13500-12
Yap, Eng-Hui; Rosche, Tyler; Almo, Steve et al. (2014) Functional clustering of immunoglobulin superfamily proteins with protein-protein interaction information calibrated hidden Markov model sequence profiles. J Mol Biol 426:945-61
Khafizov, Kamil; Madrid-Aliste, Carlos; Almo, Steven C et al. (2014) Trends in structural coverage of the protein universe and the impact of the Protein Structure Initiative. Proc Natl Acad Sci U S A 111:3733-8
Rubinstein, Rotem; Ramagopal, Udupi A; Nathenson, Stanley G et al. (2013) Functional classification of immune regulatory proteins. Structure 21:766-76
Menon, Vilas; Vallat, Brinda K; Dybas, Joseph M et al. (2013) Modeling proteins using a super-secondary structure library and NMR chemical shift information. Structure 21:891-9
Pujato, Mario; MacCarthy, Thomas; Fiser, Andras et al. (2013) The underlying molecular and network level mechanisms in the evolution of robustness in gene regulatory networks. PLoS Comput Biol 9:e1002865
Fajardo, J Eduardo; Fiser, Andras (2013) Protein structure based prediction of catalytic residues. BMC Bioinformatics 14:63
Fernandez-Fuentes, Narcis; Fiser, Andras (2013) A modular perspective of protein structures: application to fragment based loop modeling. Methods Mol Biol 932:141-58

Showing the most recent 10 out of 16 publications