Abstract

Proteins that control the transport of electrons, protons and ions underpin basic functions of living cells and are crucial to many life processes. For example, electron transfer (ET) and proton transport (PTR) combine to produce electrochemical gradients across membranes, which are then used to produce ATP. Similarly, ion channels play a vital role in neural signal transduction and other functions. Since mutations that disrupt the action of such proteins are associated with many diseases, these proteins present major targets for therapeutic intervention and play a central role in drug discovery efforts. However, further advances in rational drug development should be helped significantly by augmenting the progress in structural and biochemical studies by approaches that would provide the needed quantitative structure- function correlations. Thus, it is important to develop, refine and apply quantitative computer simulations tools for this purpose. Major progress in method development and validation, as well as pilot studies of key systems have placed this research effort in a pivotal position, where it can progress in providing quantitative structure function correlations of PTR, ion transport and ET. Thus, parallel advances in following directions are proposed:
Aim 1 - Biological PTR - The method developed in the grant allows one to quantify the action of key proton-conducting systems. Thus, the proposed projects include: (i) Exploring the gating mechanism of the Cytochrome C oxidase (CcO), while focusing on well-defined proton channels. (ii) Our recent breakthrough in modeling the conversion of pH gradients to vectorial rotation in the F0-ATPase will be quantified, striving to gain a better understanding of the proton paths. (iii) The voltage activated PTR in Hv1 will be explored (iv) The progress in coarse grained (CG) modeling of the membrane potential will be exploited in interpreting the observed relationship between the effect of the membrane potential and the PT paths in CcO. (v) The study of the early PTR in bacteriorhodopsin will be extended, focusing on subsequent steps.
Aim 2 - Biological control of ion transport - Our advances in CG modeling of the membrane potential will be exploited in further studies of the action of voltage-activated ion channels and the control of selectivity of ion channels.
Aim3 - ET Processes - ET and ET/PT in CcO will be explored.
Aim4 - Validations - Crucial validation of the different models will be conducted.

Public Health Relevance

Charge transport proteins that control the transport of electrons, protons and ions play a crucial role in life processes. Mutations that disrupt the function of such systems are associated with major diseases, including neural disorders, diabetes, cardiac arrhythmia, cancer, osteoporosis and ulcers. The charge transfer proteins present major targets for therapeutic intervention and play a central role in drug discovery efforts. However, exploiting such possibilities requires the ability to convert structural informaton to a detailed understanding of the corresponding functions. We believe that computer modeling approaches can provide the needed structure-function correlations, and thus propose to continue to push the frontiers in modeling the actual function of proton transfer, electron transfe and ion transfer proteins. The proposed studies should provide a better understanding of the molecular origin of the different modes of biological charge transport. This should provide a major help in rational development of effective drugs that will accelerate the progress in fighting diseases associated with defective charge transport systems.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
4R01GM040283-29
Application #
9122427
Study Section
Macromolecular Structure and Function D Study Section (MSFD)
Program Officer
Wehrle, Janna P
Project Start
1988-07-01
Project End
2017-07-31
Budget Start
2016-08-01
Budget End
2017-07-31
Support Year
29
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
University of Southern California
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
072933393
City
Los Angeles
State
CA
Country
United States
Zip Code
90032

  Publications

Mukherjee, Shayantani; Warshel, Arieh (2017) The FOF1 ATP synthase: from atomistic three-dimensional structure to the rotary-chemical function. Photosynth Res 134:1-15
Yoon, Hanwool; Kolev, Vesselin; Warshel, Arieh (2017) Validating the Water Flooding Approach by Comparing It to Grand Canonical Monte Carlo Simulations. J Phys Chem B 121:9358-9365
Astumian, R Dean; Mukherjee, Shayantani; Warshel, Arieh (2016) The Physics and Physical Chemistry of Molecular Machines. Chemphyschem 17:1719-41
Kim, Ilsoo; Warshel, Arieh (2016) Analyzing the electrogenicity of cytochrome c oxidase. Proc Natl Acad Sci U S A 113:7810-5
Matute, Ricardo A; Yoon, Hanwool; Warshel, Arieh (2016) Exploring the mechanism of DNA polymerases by analyzing the effect of mutations of active site acidic groups in Polymerase ?. Proteins 84:1644-1657
Alhadeff, Raphael; Warshel, Arieh (2016) Simulating the Function of the MjNhaP1 Transporter. J Phys Chem B :
Yoon, Hanwool; Warshel, Arieh (2016) The control of the discrimination between dNTP and rNTP in DNA and RNA polymerase. Proteins 84:1616-1624
Kim, Ilsoo; Warshel, Arieh (2016) A Microscopic Capacitor Model of Voltage Coupling in Membrane Proteins: Gating Charge Fluctuations in Ci-VSD. J Phys Chem B 120:418-32
Vorobyov, Igor; Kim, Ilsoo; Chu, Zhen T et al. (2016) Refining the treatment of membrane proteins by coarse-grained models. Proteins 84:92-117
Kim, Ilsoo; Warshel, Arieh (2015) Equilibrium fluctuation relations for voltage coupling in membrane proteins. Biochim Biophys Acta 1848:2985-97

Showing the most recent 10 out of 65 publications