Structural analysis on mutation residues and interfacial water molecules for human TIM disease understanding

BACKGROUND: Human triosephosphate isomerase (HsTIM) deficiency is a genetic disease caused often by the pathogenic mutation E104D. This mutation, located at the side of an abnormally large cluster of water in the inter-subunit interface, reduces the thermostability of the enzyme. Why and how these w...

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Autores principales: Li, Zhenhua, He, Ying, Liu, Qian, Zhao, Liang, Wong, Limsoon, Kwoh, Chee Keong, Nguyen, Hung, Li, Jinyan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3853089/
https://www.ncbi.nlm.nih.gov/pubmed/24564410
http://dx.doi.org/10.1186/1471-2105-14-S16-S11
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author Li, Zhenhua
He, Ying
Liu, Qian
Zhao, Liang
Wong, Limsoon
Kwoh, Chee Keong
Nguyen, Hung
Li, Jinyan
author_facet Li, Zhenhua
He, Ying
Liu, Qian
Zhao, Liang
Wong, Limsoon
Kwoh, Chee Keong
Nguyen, Hung
Li, Jinyan
author_sort Li, Zhenhua
collection PubMed
description BACKGROUND: Human triosephosphate isomerase (HsTIM) deficiency is a genetic disease caused often by the pathogenic mutation E104D. This mutation, located at the side of an abnormally large cluster of water in the inter-subunit interface, reduces the thermostability of the enzyme. Why and how these water molecules are directly related to the excessive thermolability of the mutant have not been investigated in structural biology. RESULTS: This work compares the structure of the E104D mutant with its wild type counterparts. It is found that the water topology in the dimer interface of HsTIM is atypical, having a "wet-core-dry-rim" distribution with 16 water molecules tightly packed in a small deep region surrounded by 22 residues including GLU104. These water molecules are co-conserved with their surrounding residues in non-archaeal TIMs (dimers) but not conserved across archaeal TIMs (tetramers), indicating their importance in preserving the overall quaternary structure. As the structural permutation induced by the mutation is not significant, we hypothesize that the excessive thermolability of the E104D mutant is attributed to the easy propagation of atoms' flexibility from the surface into the core via the large cluster of water. It is indeed found that the B factor increment in the wet region is higher than other regions, and, more importantly, the B factor increment in the wet region is maintained in the deeply buried core. Molecular dynamics simulations revealed that for the mutant structure at normal temperature, a clear increase of the root-mean-square deviation is observed for the wet region contacting with the large cluster of interfacial water. Such increase is not observed for other interfacial regions or the whole protein. This clearly suggests that, in the E104D mutant, the large water cluster is responsible for the subunit interface flexibility and overall thermolability, and it ultimately leads to the deficiency of this enzyme. CONCLUSIONS: Our study reveals that a large cluster of water buried in protein interfaces is fragile and high-maintenance, closely related to the structure, function and evolution of the whole protein.
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spelling pubmed-38530892013-12-16 Structural analysis on mutation residues and interfacial water molecules for human TIM disease understanding Li, Zhenhua He, Ying Liu, Qian Zhao, Liang Wong, Limsoon Kwoh, Chee Keong Nguyen, Hung Li, Jinyan BMC Bioinformatics Research BACKGROUND: Human triosephosphate isomerase (HsTIM) deficiency is a genetic disease caused often by the pathogenic mutation E104D. This mutation, located at the side of an abnormally large cluster of water in the inter-subunit interface, reduces the thermostability of the enzyme. Why and how these water molecules are directly related to the excessive thermolability of the mutant have not been investigated in structural biology. RESULTS: This work compares the structure of the E104D mutant with its wild type counterparts. It is found that the water topology in the dimer interface of HsTIM is atypical, having a "wet-core-dry-rim" distribution with 16 water molecules tightly packed in a small deep region surrounded by 22 residues including GLU104. These water molecules are co-conserved with their surrounding residues in non-archaeal TIMs (dimers) but not conserved across archaeal TIMs (tetramers), indicating their importance in preserving the overall quaternary structure. As the structural permutation induced by the mutation is not significant, we hypothesize that the excessive thermolability of the E104D mutant is attributed to the easy propagation of atoms' flexibility from the surface into the core via the large cluster of water. It is indeed found that the B factor increment in the wet region is higher than other regions, and, more importantly, the B factor increment in the wet region is maintained in the deeply buried core. Molecular dynamics simulations revealed that for the mutant structure at normal temperature, a clear increase of the root-mean-square deviation is observed for the wet region contacting with the large cluster of interfacial water. Such increase is not observed for other interfacial regions or the whole protein. This clearly suggests that, in the E104D mutant, the large water cluster is responsible for the subunit interface flexibility and overall thermolability, and it ultimately leads to the deficiency of this enzyme. CONCLUSIONS: Our study reveals that a large cluster of water buried in protein interfaces is fragile and high-maintenance, closely related to the structure, function and evolution of the whole protein. BioMed Central 2013-10-22 /pmc/articles/PMC3853089/ /pubmed/24564410 http://dx.doi.org/10.1186/1471-2105-14-S16-S11 Text en Copyright © 2013 Li et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Li, Zhenhua
He, Ying
Liu, Qian
Zhao, Liang
Wong, Limsoon
Kwoh, Chee Keong
Nguyen, Hung
Li, Jinyan
Structural analysis on mutation residues and interfacial water molecules for human TIM disease understanding
title Structural analysis on mutation residues and interfacial water molecules for human TIM disease understanding
title_full Structural analysis on mutation residues and interfacial water molecules for human TIM disease understanding
title_fullStr Structural analysis on mutation residues and interfacial water molecules for human TIM disease understanding
title_full_unstemmed Structural analysis on mutation residues and interfacial water molecules for human TIM disease understanding
title_short Structural analysis on mutation residues and interfacial water molecules for human TIM disease understanding
title_sort structural analysis on mutation residues and interfacial water molecules for human tim disease understanding
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3853089/
https://www.ncbi.nlm.nih.gov/pubmed/24564410
http://dx.doi.org/10.1186/1471-2105-14-S16-S11
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