Application of molecular dynamics simulation in the study of protein structure and function

Application of molecular dynamics simulation in the study of protein structure and function

Molecular dynamic (MD) simulation is a powerful theoretical tool which equips users with the ability to study the structures and functions of proteins by monitoring the intricate dynamics of proteins at the atomic level. With the utilization of MD simulation, dynamic processes occurring in the biolo...

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Main Author: Siti Raudah Mohamed Lazim
Other Authors: Zhang Dawei
Format: Theses and Dissertations
Language:English
Published: 2015
Subjects:
DRNTU::Science::Biological sciences::Molecular biology
Online Access:https://hdl.handle.net/10356/62909
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-629092023-02-28T23:47:02Z Application of molecular dynamics simulation in the study of protein structure and function Siti Raudah Mohamed Lazim Zhang Dawei School of Physical and Mathematical Sciences DRNTU::Science::Biological sciences::Molecular biology Molecular dynamic (MD) simulation is a powerful theoretical tool which equips users with the ability to study the structures and functions of proteins by monitoring the intricate dynamics of proteins at the atomic level. With the utilization of MD simulation, dynamic processes occurring in the biological system such as protein folding and unfolding can be examined in great detail. In this thesis, the use of MD simulation in the dynamical study of protein folding and changes in protein conformations will be discussed. In addition, the predictive power of MD simulation will also be highlighted through two studies involving the determination of the stability of apomyoglobin variants and the reduction potential of rubredoxin. Besides its application, this thesis will also bring attention to a limitation of MD simulation which is the lack of polarization energy terms in classical force fields that effectively describe the inhomogeneous electrostatic properties of proteins. The important role of polarization effect in effectively modeling protein folding will be demonstrated through a study concerning the folding of a helical peptide, 2KHK. The folding of 2KHK close to its NMR structure was observed when polarization effects of hydrogen bonds were considered through an on-the-fly charge scheme termed adaptive hydrogen bond-specific charge (AHBC) scheme while a non-native structure was attained when non-polarized force field was used. The AHBC scheme periodically updates the charges of amino acids involve in hydrogen bonding hence incorporating into the force field the variation in charge distribution between hydrogen bond pairs upon formation/disruption of hydrogen bonds. This effectively represents the changes in the protein environment arising from the rapid configurational changes of proteins during folding. The significance of electrostatic environment in accurately determining the reduction potential of rubredoxin will also be illustrated in this thesis through the use of two charge derivation schemes which differ in terms of the number of amino acid residues included during quantum mechanical calculations. From this study, a greater consideration of the electrostatic environment surrounding the iron atom of rubredoxin led to predictions which approached the experimentally determined reduction potentials. Also, the ability of the basic force field to model proteins will be portrayed through simple simulations that have been conducted to examine the conformational change of a protein from α/4β-fold to 3α-fold and to determine the stability of apomyoglobin upon mutation. Combined with appropriate tools for data analysis, MD simulations conducted were able to provide insights on the dynamics involved during the conformational change from α/4β-fold to 3α-fold and predict the stability of apomyoglobin variants relative to a wild type protein with reasonable agreement to experiment. DOCTOR OF PHILOSOPHY (SPMS) 2015-05-04T00:57:08Z 2015-05-04T00:57:08Z 2015 2015 Thesis Siti Raudah Mohamed Lazim. (2015). Application of molecular dynamics simulation in the study of protein structure and function. Doctoral thesis, Nanyang Technological University, Singapore. https://hdl.handle.net/10356/62909 10.32657/10356/62909 en 179 p. application/pdf
institution Nanyang Technological University
building NTU Library
continent Asia
country Singapore
Singapore
content_provider NTU Library
collection DR-NTU
language English
topic DRNTU::Science::Biological sciences::Molecular biology
spellingShingle DRNTU::Science::Biological sciences::Molecular biology
Siti Raudah Mohamed Lazim
Application of molecular dynamics simulation in the study of protein structure and function
description Molecular dynamic (MD) simulation is a powerful theoretical tool which equips users with the ability to study the structures and functions of proteins by monitoring the intricate dynamics of proteins at the atomic level. With the utilization of MD simulation, dynamic processes occurring in the biological system such as protein folding and unfolding can be examined in great detail. In this thesis, the use of MD simulation in the dynamical study of protein folding and changes in protein conformations will be discussed. In addition, the predictive power of MD simulation will also be highlighted through two studies involving the determination of the stability of apomyoglobin variants and the reduction potential of rubredoxin. Besides its application, this thesis will also bring attention to a limitation of MD simulation which is the lack of polarization energy terms in classical force fields that effectively describe the inhomogeneous electrostatic properties of proteins. The important role of polarization effect in effectively modeling protein folding will be demonstrated through a study concerning the folding of a helical peptide, 2KHK. The folding of 2KHK close to its NMR structure was observed when polarization effects of hydrogen bonds were considered through an on-the-fly charge scheme termed adaptive hydrogen bond-specific charge (AHBC) scheme while a non-native structure was attained when non-polarized force field was used. The AHBC scheme periodically updates the charges of amino acids involve in hydrogen bonding hence incorporating into the force field the variation in charge distribution between hydrogen bond pairs upon formation/disruption of hydrogen bonds. This effectively represents the changes in the protein environment arising from the rapid configurational changes of proteins during folding. The significance of electrostatic environment in accurately determining the reduction potential of rubredoxin will also be illustrated in this thesis through the use of two charge derivation schemes which differ in terms of the number of amino acid residues included during quantum mechanical calculations. From this study, a greater consideration of the electrostatic environment surrounding the iron atom of rubredoxin led to predictions which approached the experimentally determined reduction potentials. Also, the ability of the basic force field to model proteins will be portrayed through simple simulations that have been conducted to examine the conformational change of a protein from α/4β-fold to 3α-fold and to determine the stability of apomyoglobin upon mutation. Combined with appropriate tools for data analysis, MD simulations conducted were able to provide insights on the dynamics involved during the conformational change from α/4β-fold to 3α-fold and predict the stability of apomyoglobin variants relative to a wild type protein with reasonable agreement to experiment.
author2 Zhang Dawei
author_facet Zhang Dawei
Siti Raudah Mohamed Lazim
format Theses and Dissertations
author Siti Raudah Mohamed Lazim
author_sort Siti Raudah Mohamed Lazim
title Application of molecular dynamics simulation in the study of protein structure and function
title_short Application of molecular dynamics simulation in the study of protein structure and function
title_full Application of molecular dynamics simulation in the study of protein structure and function
title_fullStr Application of molecular dynamics simulation in the study of protein structure and function
title_full_unstemmed Application of molecular dynamics simulation in the study of protein structure and function
title_sort application of molecular dynamics simulation in the study of protein structure and function
publishDate 2015
url https://hdl.handle.net/10356/62909
_version_ 1759855847181123584

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