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GPU accelerated molecular dynamics simulations for protein-protein interaction of ankyrin complex

The ankyrin repeat (AR) can be used as a versatile scaffold for protein-protein interactions. It consists of a 33-residues sequence motif found in proteins with diverse functions, such as transcription initiation, cell cycle regulation, cytoskeletal integrity, ion transport, and cell-cell signaling....

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Main Authors: Kodchakorn, K., Dokmaisrijan, S., Chong, W.L., Payaka, A., Wisitponchai, T., Nimmanpipug, P., Zain, S.M., Rahman, N.A., Tayapiwatana, C., Lee, V.S.
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Published: 2018
Online Access:http://dspace.uniten.edu.my/jspui/handle/123456789/9751
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spelling my.uniten.dspace-97512018-03-06T03:49:24Z GPU accelerated molecular dynamics simulations for protein-protein interaction of ankyrin complex Kodchakorn, K. Dokmaisrijan, S. Chong, W.L. Payaka, A. Wisitponchai, T. Nimmanpipug, P. Zain, S.M. Rahman, N.A. Tayapiwatana, C. Lee, V.S. The ankyrin repeat (AR) can be used as a versatile scaffold for protein-protein interactions. It consists of a 33-residues sequence motif found in proteins with diverse functions, such as transcription initiation, cell cycle regulation, cytoskeletal integrity, ion transport, and cell-cell signaling. Using AR with high affinity for the Escherichia coli maltose binding protein (MBP) as our model system, we explored a structure-based computational protocol to probe and characterize binding affinity hot-spots at protein-protein interfaces. In this study, the long time scale dynamics simulations with GPU accelerated molecular dynamics (MD) simulations in AMBER12 have been performed to locate the hot-spots of protein-protein interaction by the analysis of the Molecular Mechanics-Poisson-Boltzmann Surface Area/Generalized Born Solvent Area (MM-PBSA/GBSA) of the MD trajectories. The two designed AR systems with different binding affinities from ELISA were simulated. Our calculations gave the absolute binding affinity predictions which are in agreement with the kinetic experiment. The difference in binding affinity of the two selected clones is due to the framework mutations which are mostly conserved at a β-hairpin/loop region. AR domain is most probably not affected by the alteration of this framework from the long time scale MDs. © 2014 Taylor & Francis Group, LLC. 2018-03-06T03:49:24Z 2018-03-06T03:49:24Z 2014 http://dspace.uniten.edu.my/jspui/handle/123456789/9751
institution Universiti Tenaga Nasional
building UNITEN Library
collection Institutional Repository
continent Asia
country Malaysia
content_provider Universiti Tenaga Nasional
content_source UNITEN Institutional Repository
url_provider http://dspace.uniten.edu.my/
description The ankyrin repeat (AR) can be used as a versatile scaffold for protein-protein interactions. It consists of a 33-residues sequence motif found in proteins with diverse functions, such as transcription initiation, cell cycle regulation, cytoskeletal integrity, ion transport, and cell-cell signaling. Using AR with high affinity for the Escherichia coli maltose binding protein (MBP) as our model system, we explored a structure-based computational protocol to probe and characterize binding affinity hot-spots at protein-protein interfaces. In this study, the long time scale dynamics simulations with GPU accelerated molecular dynamics (MD) simulations in AMBER12 have been performed to locate the hot-spots of protein-protein interaction by the analysis of the Molecular Mechanics-Poisson-Boltzmann Surface Area/Generalized Born Solvent Area (MM-PBSA/GBSA) of the MD trajectories. The two designed AR systems with different binding affinities from ELISA were simulated. Our calculations gave the absolute binding affinity predictions which are in agreement with the kinetic experiment. The difference in binding affinity of the two selected clones is due to the framework mutations which are mostly conserved at a β-hairpin/loop region. AR domain is most probably not affected by the alteration of this framework from the long time scale MDs. © 2014 Taylor & Francis Group, LLC.
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author Kodchakorn, K.
Dokmaisrijan, S.
Chong, W.L.
Payaka, A.
Wisitponchai, T.
Nimmanpipug, P.
Zain, S.M.
Rahman, N.A.
Tayapiwatana, C.
Lee, V.S.
spellingShingle Kodchakorn, K.
Dokmaisrijan, S.
Chong, W.L.
Payaka, A.
Wisitponchai, T.
Nimmanpipug, P.
Zain, S.M.
Rahman, N.A.
Tayapiwatana, C.
Lee, V.S.
GPU accelerated molecular dynamics simulations for protein-protein interaction of ankyrin complex
author_facet Kodchakorn, K.
Dokmaisrijan, S.
Chong, W.L.
Payaka, A.
Wisitponchai, T.
Nimmanpipug, P.
Zain, S.M.
Rahman, N.A.
Tayapiwatana, C.
Lee, V.S.
author_sort Kodchakorn, K.
title GPU accelerated molecular dynamics simulations for protein-protein interaction of ankyrin complex
title_short GPU accelerated molecular dynamics simulations for protein-protein interaction of ankyrin complex
title_full GPU accelerated molecular dynamics simulations for protein-protein interaction of ankyrin complex
title_fullStr GPU accelerated molecular dynamics simulations for protein-protein interaction of ankyrin complex
title_full_unstemmed GPU accelerated molecular dynamics simulations for protein-protein interaction of ankyrin complex
title_sort gpu accelerated molecular dynamics simulations for protein-protein interaction of ankyrin complex
publishDate 2018
url http://dspace.uniten.edu.my/jspui/handle/123456789/9751
_version_ 1644494797669400576
score 13.160551

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