Abstract

Many proteins function as molecular machines. Understanding the principles that control the machinery of biomolecular systems is a computational challenge in many cases due to the involvement of macromolecular structures composed of multiple subunits and cooperative interactions manifested by allosteric changes in conformations, which are beyond the range of atomic simulations. Our goal in a recently funded R33 has been to develop and utilize low resolution models for exploring the collective dynamics of such complex systems, and bridging between structure and function, based on the paradigm structure-encodes-dynamics-encodes-function. The elastic network models and methods we introduced to this aim have found utility in many applications and helped us gain insights into the intrinsic, structure- encoded ability of proteins to favor the reconfiguration of native structures between functional substates. In the present R01, we are proposing to build on our previous work, to further explore the structure ->dynamics ->function mapping of allosteric and/or multimeric proteins using physically-based and computationally efficient models in collaboration with the NCBC Simbios at Stanford U (PI: Altman). The Simbios group has already started to construct a new simulation package, Simbody, the utility of which is expected to be significantly enhanced by a collaborative work.
Our specific aims are (1) to build models and methods for automated coarse-graining of complex structures at multiple levels of resolution and assessing their collective dynamics, toward using the resulting models (structure) and data (motions) in Simbody;(2) to complement the physics-based approach developed in Aim 1 by information-theoretic approaches toward delineating signal transduction pathways/mechanisms in allosteric systems, and establishing the connection between these pathways and structural dynamics, and (3) to gain insights into the machinery of molecular chaperones, using as prototypes the bacterial chaperonin GroEL-GroES and the DnaK chaperone system, in collaboration with the Gierasch lab currently doing NIH-supported experiments for understanding the allosteric dynamics of the DnaK system. An important outcome of this project will be the establishment of a methodology for simulating the machinery of biomolecular systems on the order of Megadaltons, which will be achieved in collaboration with the Schulten lab, in addition to our partnership with the Simbios team.

Public Health Relevance

Many proteins function as molecular machines. Understanding the dynamics or underlying molecular principles of these machines is a challenge due to the highly cooperative nature of interactions, which simultaneously involve multiple molecules. The aim of this project is twofold: to develop and implement computational models and methods to improve our understanding of the collective dynamics of proteins;and to elucidate the machinery of molecular chaperones - molecular systems that play an essential role in cellular physiology by assisting the folding and assembly/disassembly of proteins and directing them to transport and degradation pathways. These aims will be pursued in collaboration with the National Center for Biomedical Computing Simbios at Stanford U.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM086238-02
Application #
7751334
Study Section
Special Emphasis Panel (ZRG1-BST-E (50))
Program Officer
Wehrle, Janna P
Project Start
2009-01-01
Project End
2012-12-31
Budget Start
2010-01-01
Budget End
2010-12-31
Support Year
2
Fiscal Year
2010
Total Cost
$324,772
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Biology
Type
Schools of Medicine
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Eyal, Eran; Lum, Gengkon; Bahar, Ivet (2015) The anisotropic network model web server at 2015 (ANM 2.0). Bioinformatics 31:1487-9
Zomot, Elia; Gur, Mert; Bahar, Ivet (2015) Microseconds simulations reveal a new sodium-binding site and the mechanism of sodium-coupled substrate uptake by LeuT. J Biol Chem 290:544-55
Hu, Dong; Gur, Mert; Zhou, Zhuan et al. (2015) Interplay between arginine methylation and ubiquitylation regulates KLF4-mediated genome stability and carcinogenesis. Nat Commun 6:8419
Mao, Wenzhi; Kaya, Cihan; Dutta, Anindita et al. (2015) Comparative study of the effectiveness and limitations of current methods for detecting sequence coevolution. Bioinformatics 31:1929-37
Cheng, Mary Hongying; Bahar, Ivet (2014) Complete mapping of substrate translocation highlights the role of LeuT N-terminal segment in regulating transport cycle. PLoS Comput Biol 10:e1003879
LaRusch, Jessica; Jung, Jinsei; General, Ignacio J et al. (2014) Mechanisms of CFTR functional variants that impair regulated bicarbonate permeation and increase risk for pancreatitis but not for cystic fibrosis. PLoS Genet 10:e1004376
Das, Avisek; Gur, Mert; Cheng, Mary Hongying et al. (2014) Exploring the conformational transitions of biomolecular systems using a simple two-state anisotropic network model. PLoS Comput Biol 10:e1003521
Cheng, Mary Hongying; Bahar, Ivet (2013) Coupled global and local changes direct substrate translocation by neurotransmitter-sodium symporter ortholog LeuT. Biophys J 105:630-9
Huang, Grace T; Cunningham, Kathryn I; Benos, Panayiotis V et al. (2013) Spectral clustering strategies for heterogeneous disease expression data. Pac Symp Biocomput :212-23
Castro, Jason B; Ramanathan, Arvind; Chennubhotla, Chakra S (2013) Categorical dimensions of human odor descriptor space revealed by non-negative matrix factorization. PLoS One 8:e73289

Showing the most recent 10 out of 47 publications