Computational studies of natural and synthetic ion channels

This thesis addresses questions pertaining to three different systems-gemini surfactants, synthetic peptide ion channels and M2 proton channel from influenza A virus. The excellent surfactant properties of gemini surfactants enable their applications from consumer products to vectors for gene transf...

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Bibliographic Details
Main Author: Khurana, Ekta
Format: Text
Language:English
Published: ScholarlyCommons 2008
Subjects:
Chemistry
Physical|Biology
Virology|Biophysics
General
Gemini
Avian flu
Online Access:https://repository.upenn.edu/dissertations/AAI3309457
id ftunivpenn:oai:repository.upenn.edu:dissertations-7950
record_format openpolar
spelling ftunivpenn:oai:repository.upenn.edu:dissertations-7950 2023-05-15T15:34:36+02:00 Computational studies of natural and synthetic ion channels Khurana, Ekta 2008-01-01T08:00:00Z https://repository.upenn.edu/dissertations/AAI3309457 EN eng ScholarlyCommons https://repository.upenn.edu/dissertations/AAI3309457 Dissertations available from ProQuest Chemistry Physical|Biology Virology|Biophysics General text 2008 ftunivpenn 2021-01-04T21:28:28Z This thesis addresses questions pertaining to three different systems-gemini surfactants, synthetic peptide ion channels and M2 proton channel from influenza A virus. The excellent surfactant properties of gemini surfactants enable their applications from consumer products to vectors for gene transfection. The results emerging from a neutron reflection study of a series of these surfactants reveal their unusual interfacial behavior, demanding a higher resolution picture for their further exploration. Synthetic cyclic peptides self-assemble to form excellent ion channels with a wide range of potential applications ranging from nanomaterials to antimicrobial agents, but the mechanism of their self-assembly is not clear. The M2 proton channel was used regularly as a target for anti-influenza drugs before the appearance of resistant viral strains with mutated forms of M2, including the avian flu strain. Although the NMR and X-ray crystal structures reported recently have significantly advanced the understanding of M2, a complete knowledge of the drug binding to the channel required to design new drugs for the mutated forms remains incomplete. The goal of the thesis is to shed light on these uncertainties at the molecular level. Molecular dynamics (MD) simulations at different levels of details have been used as a tool to complement the experiments and answer the unresolved questions. Using atomistic simulations, we observe gemini surfactant aggregation below air-water interface explaining their unusual behavior detected by experiments. Large-scale simulations of coarse-grained (CG) cyclic peptides at a liquid-liquid interface demonstrate a likely self-assembly mechanism and pave the way to the exploration of CG models to study cyclic peptides in different environments and nanomaterials at liquid-liquid interfaces. Atomistic simulations of the transmembrane domain of M2 in DMPC bilayers reveal possible structural transitions that would occur as the channel switches between its open and closed states. The drug binding site and the orientation of the drug in the open state of the channel are confirmed to be in agreement with the one proposed by crystallographic studies, and a change in the drug orientation with the closing of the channel is proposed. In conclusion, the results of MD simulations have filled some missing gaps in the existing pictures that have emerged from experiments and in principle can be used to guide further experiments. ^ Text Avian flu University of Pennsylvania: ScholaryCommons@Penn Gemini ENVELOPE(-62.500,-62.500,-66.133,-66.133)
institution Open Polar
collection University of Pennsylvania: ScholaryCommons@Penn
op_collection_id ftunivpenn
language English
topic Chemistry
Physical|Biology
Virology|Biophysics
General
spellingShingle Chemistry
Physical|Biology
Virology|Biophysics
General
Khurana, Ekta
Computational studies of natural and synthetic ion channels
topic_facet Chemistry
Physical|Biology
Virology|Biophysics
General
description This thesis addresses questions pertaining to three different systems-gemini surfactants, synthetic peptide ion channels and M2 proton channel from influenza A virus. The excellent surfactant properties of gemini surfactants enable their applications from consumer products to vectors for gene transfection. The results emerging from a neutron reflection study of a series of these surfactants reveal their unusual interfacial behavior, demanding a higher resolution picture for their further exploration. Synthetic cyclic peptides self-assemble to form excellent ion channels with a wide range of potential applications ranging from nanomaterials to antimicrobial agents, but the mechanism of their self-assembly is not clear. The M2 proton channel was used regularly as a target for anti-influenza drugs before the appearance of resistant viral strains with mutated forms of M2, including the avian flu strain. Although the NMR and X-ray crystal structures reported recently have significantly advanced the understanding of M2, a complete knowledge of the drug binding to the channel required to design new drugs for the mutated forms remains incomplete. The goal of the thesis is to shed light on these uncertainties at the molecular level. Molecular dynamics (MD) simulations at different levels of details have been used as a tool to complement the experiments and answer the unresolved questions. Using atomistic simulations, we observe gemini surfactant aggregation below air-water interface explaining their unusual behavior detected by experiments. Large-scale simulations of coarse-grained (CG) cyclic peptides at a liquid-liquid interface demonstrate a likely self-assembly mechanism and pave the way to the exploration of CG models to study cyclic peptides in different environments and nanomaterials at liquid-liquid interfaces. Atomistic simulations of the transmembrane domain of M2 in DMPC bilayers reveal possible structural transitions that would occur as the channel switches between its open and closed states. The drug binding site and the orientation of the drug in the open state of the channel are confirmed to be in agreement with the one proposed by crystallographic studies, and a change in the drug orientation with the closing of the channel is proposed. In conclusion, the results of MD simulations have filled some missing gaps in the existing pictures that have emerged from experiments and in principle can be used to guide further experiments. ^
format Text
author Khurana, Ekta
author_facet Khurana, Ekta
author_sort Khurana, Ekta
title Computational studies of natural and synthetic ion channels
title_short Computational studies of natural and synthetic ion channels
title_full Computational studies of natural and synthetic ion channels
title_fullStr Computational studies of natural and synthetic ion channels
title_full_unstemmed Computational studies of natural and synthetic ion channels
title_sort computational studies of natural and synthetic ion channels
publisher ScholarlyCommons
publishDate 2008
url https://repository.upenn.edu/dissertations/AAI3309457
long_lat ENVELOPE(-62.500,-62.500,-66.133,-66.133)
geographic Gemini
geographic_facet Gemini
genre Avian flu
genre_facet Avian flu
op_source Dissertations available from ProQuest
op_relation https://repository.upenn.edu/dissertations/AAI3309457
_version_ 1766364940345540608

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