Membrane proteins are critical to many biological processes, including molecular transport, signal transduction, and cellular interactions. Through the use of molecular dynamics (MD) simulations, we are able to model this environment at an atomistic scale. However, traditionally used nonpolarizable force fields (FF) are thought to model the unique dielectric gradient posed by the lipid environment with a limited accuracy due to the mean field approximation of charge. Advancements in polarizable FFs and computing efficiency has enabled the explicit modeling of polarization responses and charge distribution, enabling a deeper understanding of the electrostatics driving these processes. Through the use of the Drude FF, we study three specific model systems to understand where explicit polarization is important in describing membranes and membrane proteins. These studies sought to answer the questions: (1) How does explicit electronic polarization impact small molecule permeation and localization preference?, (2) What electrostatic interactions underlie membrane protein secondary structure?, and (3) How do conformational changes propagate between microswitches in G-Protein Coupled Receptors? In this work, we show small molecule dipole moments changing as a function of localization in the bilayer. Additionally, we show differences in the free energy surfaces of permeation for aromatic, polar, and negatively charged species reliant upon force field used. For secondary structure, we showed key interactions which aided to stabilize model helices in bilayers. Finally, we showed potential inductive effects of key microswitch residues underlying prototypical G-Protein coupled receptor activation. This dissertation has helped to show the importance of including explicit polarization in membrane protein systems, especially when considering interactions at the interface and modeling species with charge. This work enables a refined view of the electrostatics occurring in membranes and membrane protein systems, and in the future, can be used as a basis for methodologies in computer aided drug design efforts. / Doctor of Philosophy / Deepening our understandings of membranes and membrane proteins enable better informed and more efficient drug design. In order to do this, biological processes can be simulated through molecular dynamics (MD) simulations. MD simulations use mathematical models known as force fields (FF) to represent the physics of biological systems at an atomistic scale. This enables the study of key interactions which can be leveraged for drug discovery efforts. However, traditional FF neglect electronic structural changes which are crucial for accurately describing the membrane environment and the influence it has on surrounding and embedded molecules. Using enhanced FFs, known as polarizable FFs, we can model this response and gain an entirely new perspective on membranes and membrane proteins. This work helps to define when these FFs are most important to be used when studying membranes and membrane proteins, and in the future, serve as a basis for further simulations in drug discovery efforts.
Identifer | oai:union.ndltd.org:VTETD/oai:vtechworks.lib.vt.edu:10919/119514 |
Date | 25 June 2024 |
Creators | Montgomery, Julia Mae |
Contributors | Biochemistry, Lemkul, Justin Alan, Vinauger Tella, Clement, Brown, Anne M., Klemba, Michael Wade |
Publisher | Virginia Tech |
Source Sets | Virginia Tech Theses and Dissertation |
Language | English |
Detected Language | English |
Type | Dissertation |
Format | ETD, application/pdf |
Rights | In Copyright, http://rightsstatements.org/vocab/InC/1.0/ |
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