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Molecular modelling of urease accessory interaction proteins of Helicobacter Pylori J 99 and predicting an interruption in interaction by Vigna radiata Defensins

Helicobacter pylori is the major causative agent of Gastric carcinoma. Significance of the urease accessory interaction proteins are emphasized in colonization of human gastric mucosa and efficient infection of H. pylori. Here an attempt is made to explore the structure and properties of urease acce...

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Autores principales: Paramasivan, Manivannan, Sankaran, Ganesan, Sethuraman, Naveenkumar, Devadoss, Daniel Selvakumar, Thangavelu, Sathiamoorthi, Gangatharan, Muralitharan
Formato: Texto
Lenguaje:English
Publicado: Biomedical Informatics 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3055154/
https://www.ncbi.nlm.nih.gov/pubmed/21423886
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author Paramasivan, Manivannan
Sankaran, Ganesan
Sethuraman, Naveenkumar
Devadoss, Daniel Selvakumar
Thangavelu, Sathiamoorthi
Gangatharan, Muralitharan
author_facet Paramasivan, Manivannan
Sankaran, Ganesan
Sethuraman, Naveenkumar
Devadoss, Daniel Selvakumar
Thangavelu, Sathiamoorthi
Gangatharan, Muralitharan
author_sort Paramasivan, Manivannan
collection PubMed
description Helicobacter pylori is the major causative agent of Gastric carcinoma. Significance of the urease accessory interaction proteins are emphasized in colonization of human gastric mucosa and efficient infection of H. pylori. Here an attempt is made to explore the structure and properties of urease accessory interaction proteins from Helicobacter pylori J 99. The proteins chosen for the study are ureH, ureI, nikR, groL and flgS based on the interaction map available from STRING database. The above mentioned proteins do not have a comprehensive three dimensional structure. Hence the models were generated using PSI-BLAST (Position Specific Iterative-Blast) and MODELLER 9V8. Physicochemical characterization encompasses pI, EC, AI, II and GRAVY. Secondary structure was predicted using PSI-PRED. Functional characterization was done by SOSUI and DISULFIND Servers and refinement of structure was done using Ramachandran plot analysis. RMS-Z values were calculated using Q-MEAN Server and CHIMERA was used for molecular simulation studies. Plant defensins from Vigna radiata are successfully docked to the modeled structures and thus interaction could be possibly prevented. These results will pave way for further selective inhibition of H. pylori colonization and in vivo survival by employing plant defensins from Vigna radiata (VrD1 & VrD2). The work will prove that plant defensins provides anticancer relief too.
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spelling pubmed-30551542011-03-18 Molecular modelling of urease accessory interaction proteins of Helicobacter Pylori J 99 and predicting an interruption in interaction by Vigna radiata Defensins Paramasivan, Manivannan Sankaran, Ganesan Sethuraman, Naveenkumar Devadoss, Daniel Selvakumar Thangavelu, Sathiamoorthi Gangatharan, Muralitharan Bioinformation Hypothesis Helicobacter pylori is the major causative agent of Gastric carcinoma. Significance of the urease accessory interaction proteins are emphasized in colonization of human gastric mucosa and efficient infection of H. pylori. Here an attempt is made to explore the structure and properties of urease accessory interaction proteins from Helicobacter pylori J 99. The proteins chosen for the study are ureH, ureI, nikR, groL and flgS based on the interaction map available from STRING database. The above mentioned proteins do not have a comprehensive three dimensional structure. Hence the models were generated using PSI-BLAST (Position Specific Iterative-Blast) and MODELLER 9V8. Physicochemical characterization encompasses pI, EC, AI, II and GRAVY. Secondary structure was predicted using PSI-PRED. Functional characterization was done by SOSUI and DISULFIND Servers and refinement of structure was done using Ramachandran plot analysis. RMS-Z values were calculated using Q-MEAN Server and CHIMERA was used for molecular simulation studies. Plant defensins from Vigna radiata are successfully docked to the modeled structures and thus interaction could be possibly prevented. These results will pave way for further selective inhibition of H. pylori colonization and in vivo survival by employing plant defensins from Vigna radiata (VrD1 & VrD2). The work will prove that plant defensins provides anticancer relief too. Biomedical Informatics 2011-02-15 /pmc/articles/PMC3055154/ /pubmed/21423886 Text en © 2011 Biomedical Informatics This is an open-access article, which permits unrestricted use, distribution, and reproduction in any medium, for non-commercial purposes, provided the original author and source are credited.
spellingShingle Hypothesis
Paramasivan, Manivannan
Sankaran, Ganesan
Sethuraman, Naveenkumar
Devadoss, Daniel Selvakumar
Thangavelu, Sathiamoorthi
Gangatharan, Muralitharan
Molecular modelling of urease accessory interaction proteins of Helicobacter Pylori J 99 and predicting an interruption in interaction by Vigna radiata Defensins
title Molecular modelling of urease accessory interaction proteins of Helicobacter Pylori J 99 and predicting an interruption in interaction by Vigna radiata Defensins
title_full Molecular modelling of urease accessory interaction proteins of Helicobacter Pylori J 99 and predicting an interruption in interaction by Vigna radiata Defensins
title_fullStr Molecular modelling of urease accessory interaction proteins of Helicobacter Pylori J 99 and predicting an interruption in interaction by Vigna radiata Defensins
title_full_unstemmed Molecular modelling of urease accessory interaction proteins of Helicobacter Pylori J 99 and predicting an interruption in interaction by Vigna radiata Defensins
title_short Molecular modelling of urease accessory interaction proteins of Helicobacter Pylori J 99 and predicting an interruption in interaction by Vigna radiata Defensins
title_sort molecular modelling of urease accessory interaction proteins of helicobacter pylori j 99 and predicting an interruption in interaction by vigna radiata defensins
topic Hypothesis
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3055154/
https://www.ncbi.nlm.nih.gov/pubmed/21423886
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