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Comparative modeling of CCRL1, a key protein in masked immune diseases and virtual screening for finding inhibitor of this protein

Human CCRL1 belongs to the family of silent chemokine receptors. This transmembrane protein plays a role in blunting function of chemokines through binding to them. This will attenuate immune responses. Interaction between CCRL1 and CCL21 determines this immune extinction. Thus inhibiting the action...

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Autores principales: Behjati, Mohaddeseh, Torktaz, Ibrahim, Mohammadpour, Mehrdad, Ahmadian, Gholamreza, Easton, Andrew J
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Biomedical Informatics 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3338979/
https://www.ncbi.nlm.nih.gov/pubmed/22553392
http://dx.doi.org/10.6026/97320630008336
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author Behjati, Mohaddeseh
Torktaz, Ibrahim
Mohammadpour, Mehrdad
Ahmadian, Gholamreza
Easton, Andrew J
author_facet Behjati, Mohaddeseh
Torktaz, Ibrahim
Mohammadpour, Mehrdad
Ahmadian, Gholamreza
Easton, Andrew J
author_sort Behjati, Mohaddeseh
collection PubMed
description Human CCRL1 belongs to the family of silent chemokine receptors. This transmembrane protein plays a role in blunting function of chemokines through binding to them. This will attenuate immune responses. Interaction between CCRL1 and CCL21 determines this immune extinction. Thus inhibiting the action of this atypical chemokine seems to stimulate immune responses especially in the case of suppressed and immune deficient conditions. In this study we predicted 3D structure of CCRL1 using comparative modeling and Hiddebn Markov Model algorithm. Final predicted model optimized by Modeller v9.8 and minimized regarding energy level using UCSF chimera candidate version1.5.3. ClasPro webserver was used to find interacting residues between CCRL1 and CCL21. Interacting residues were used as target for chemical inhibitors by simulated docking study. For finding potential inhibitors, library of KEGG compounds screened and 97 obtained chemicals docked against interacting residues between CCRL1- CCL21 and MolDock was used as docking scoring function. Results indicated that Hexadecanal is a potential inhibitor of CCRL1- CCL21 interaction. Inhibition of this interaction will increase intercellular level of CCl21 and interaction between CCL21 and CCR7 causes immune potentiaiton.
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spelling pubmed-33389792012-05-02 Comparative modeling of CCRL1, a key protein in masked immune diseases and virtual screening for finding inhibitor of this protein Behjati, Mohaddeseh Torktaz, Ibrahim Mohammadpour, Mehrdad Ahmadian, Gholamreza Easton, Andrew J Bioinformation Hypothesis Human CCRL1 belongs to the family of silent chemokine receptors. This transmembrane protein plays a role in blunting function of chemokines through binding to them. This will attenuate immune responses. Interaction between CCRL1 and CCL21 determines this immune extinction. Thus inhibiting the action of this atypical chemokine seems to stimulate immune responses especially in the case of suppressed and immune deficient conditions. In this study we predicted 3D structure of CCRL1 using comparative modeling and Hiddebn Markov Model algorithm. Final predicted model optimized by Modeller v9.8 and minimized regarding energy level using UCSF chimera candidate version1.5.3. ClasPro webserver was used to find interacting residues between CCRL1 and CCL21. Interacting residues were used as target for chemical inhibitors by simulated docking study. For finding potential inhibitors, library of KEGG compounds screened and 97 obtained chemicals docked against interacting residues between CCRL1- CCL21 and MolDock was used as docking scoring function. Results indicated that Hexadecanal is a potential inhibitor of CCRL1- CCL21 interaction. Inhibition of this interaction will increase intercellular level of CCl21 and interaction between CCL21 and CCR7 causes immune potentiaiton. Biomedical Informatics 2012-04-13 /pmc/articles/PMC3338979/ /pubmed/22553392 http://dx.doi.org/10.6026/97320630008336 Text en © 2012 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
Behjati, Mohaddeseh
Torktaz, Ibrahim
Mohammadpour, Mehrdad
Ahmadian, Gholamreza
Easton, Andrew J
Comparative modeling of CCRL1, a key protein in masked immune diseases and virtual screening for finding inhibitor of this protein
title Comparative modeling of CCRL1, a key protein in masked immune diseases and virtual screening for finding inhibitor of this protein
title_full Comparative modeling of CCRL1, a key protein in masked immune diseases and virtual screening for finding inhibitor of this protein
title_fullStr Comparative modeling of CCRL1, a key protein in masked immune diseases and virtual screening for finding inhibitor of this protein
title_full_unstemmed Comparative modeling of CCRL1, a key protein in masked immune diseases and virtual screening for finding inhibitor of this protein
title_short Comparative modeling of CCRL1, a key protein in masked immune diseases and virtual screening for finding inhibitor of this protein
title_sort comparative modeling of ccrl1, a key protein in masked immune diseases and virtual screening for finding inhibitor of this protein
topic Hypothesis
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3338979/
https://www.ncbi.nlm.nih.gov/pubmed/22553392
http://dx.doi.org/10.6026/97320630008336
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