Identification of a Novel Drug Lead That Inhibits HCV Infection and Cell-to-Cell Transmission by Targeting the HCV E2 Glycoprotein

Hepatitis C Virus (HCV) infects 200 million individuals worldwide. Although several FDA approved drugs targeting the HCV serine protease and polymerase have shown promising results, there is a need for better drugs that are effective in treating a broader range of HCV genotypes and subtypes without...

Descripción completa

Detalles Bibliográficos
Autores principales: Al Olaby, Reem R., Cocquerel, Laurence, Zemla, Adam, Saas, Laure, Dubuisson, Jean, Vielmetter, Jost, Marcotrigiano, Joseph, Khan, Abdul Ghafoor, Catalan, Felipe Vences, Perryman, Alexander L., Freundlich, Joel S., Forli, Stefano, Levy, Shoshana, Balhorn, Rod, Azzazy, Hassan M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4214736/
https://www.ncbi.nlm.nih.gov/pubmed/25357246
http://dx.doi.org/10.1371/journal.pone.0111333
_version_ 1782342004411203584
author Al Olaby, Reem R.
Cocquerel, Laurence
Zemla, Adam
Saas, Laure
Dubuisson, Jean
Vielmetter, Jost
Marcotrigiano, Joseph
Khan, Abdul Ghafoor
Catalan, Felipe Vences
Perryman, Alexander L.
Freundlich, Joel S.
Forli, Stefano
Levy, Shoshana
Balhorn, Rod
Azzazy, Hassan M.
author_facet Al Olaby, Reem R.
Cocquerel, Laurence
Zemla, Adam
Saas, Laure
Dubuisson, Jean
Vielmetter, Jost
Marcotrigiano, Joseph
Khan, Abdul Ghafoor
Catalan, Felipe Vences
Perryman, Alexander L.
Freundlich, Joel S.
Forli, Stefano
Levy, Shoshana
Balhorn, Rod
Azzazy, Hassan M.
author_sort Al Olaby, Reem R.
collection PubMed
description Hepatitis C Virus (HCV) infects 200 million individuals worldwide. Although several FDA approved drugs targeting the HCV serine protease and polymerase have shown promising results, there is a need for better drugs that are effective in treating a broader range of HCV genotypes and subtypes without being used in combination with interferon and/or ribavirin. Recently, two crystal structures of the core of the HCV E2 protein (E2c) have been determined, providing structural information that can now be used to target the E2 protein and develop drugs that disrupt the early stages of HCV infection by blocking E2’s interaction with different host factors. Using the E2c structure as a template, we have created a structural model of the E2 protein core (residues 421–645) that contains the three amino acid segments that are not present in either structure. Computational docking of a diverse library of 1,715 small molecules to this model led to the identification of a set of 34 ligands predicted to bind near conserved amino acid residues involved in the HCV E2: CD81 interaction. Surface plasmon resonance detection was used to screen the ligand set for binding to recombinant E2 protein, and the best binders were subsequently tested to identify compounds that inhibit the infection of Huh-7 cells by HCV. One compound, 281816, blocked E2 binding to CD81 and inhibited HCV infection in a genotype-independent manner with IC50’s ranging from 2.2 µM to 4.6 µM. 281816 blocked the early and late steps of cell-free HCV entry and also abrogated the cell-to-cell transmission of HCV. Collectively the results obtained with this new structural model of E2c suggest the development of small molecule inhibitors such as 281816 that target E2 and disrupt its interaction with CD81 may provide a new paradigm for HCV treatment.
format Online
Article
Text
id pubmed-4214736
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-42147362014-11-05 Identification of a Novel Drug Lead That Inhibits HCV Infection and Cell-to-Cell Transmission by Targeting the HCV E2 Glycoprotein Al Olaby, Reem R. Cocquerel, Laurence Zemla, Adam Saas, Laure Dubuisson, Jean Vielmetter, Jost Marcotrigiano, Joseph Khan, Abdul Ghafoor Catalan, Felipe Vences Perryman, Alexander L. Freundlich, Joel S. Forli, Stefano Levy, Shoshana Balhorn, Rod Azzazy, Hassan M. PLoS One Research Article Hepatitis C Virus (HCV) infects 200 million individuals worldwide. Although several FDA approved drugs targeting the HCV serine protease and polymerase have shown promising results, there is a need for better drugs that are effective in treating a broader range of HCV genotypes and subtypes without being used in combination with interferon and/or ribavirin. Recently, two crystal structures of the core of the HCV E2 protein (E2c) have been determined, providing structural information that can now be used to target the E2 protein and develop drugs that disrupt the early stages of HCV infection by blocking E2’s interaction with different host factors. Using the E2c structure as a template, we have created a structural model of the E2 protein core (residues 421–645) that contains the three amino acid segments that are not present in either structure. Computational docking of a diverse library of 1,715 small molecules to this model led to the identification of a set of 34 ligands predicted to bind near conserved amino acid residues involved in the HCV E2: CD81 interaction. Surface plasmon resonance detection was used to screen the ligand set for binding to recombinant E2 protein, and the best binders were subsequently tested to identify compounds that inhibit the infection of Huh-7 cells by HCV. One compound, 281816, blocked E2 binding to CD81 and inhibited HCV infection in a genotype-independent manner with IC50’s ranging from 2.2 µM to 4.6 µM. 281816 blocked the early and late steps of cell-free HCV entry and also abrogated the cell-to-cell transmission of HCV. Collectively the results obtained with this new structural model of E2c suggest the development of small molecule inhibitors such as 281816 that target E2 and disrupt its interaction with CD81 may provide a new paradigm for HCV treatment. Public Library of Science 2014-10-30 /pmc/articles/PMC4214736/ /pubmed/25357246 http://dx.doi.org/10.1371/journal.pone.0111333 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Al Olaby, Reem R.
Cocquerel, Laurence
Zemla, Adam
Saas, Laure
Dubuisson, Jean
Vielmetter, Jost
Marcotrigiano, Joseph
Khan, Abdul Ghafoor
Catalan, Felipe Vences
Perryman, Alexander L.
Freundlich, Joel S.
Forli, Stefano
Levy, Shoshana
Balhorn, Rod
Azzazy, Hassan M.
Identification of a Novel Drug Lead That Inhibits HCV Infection and Cell-to-Cell Transmission by Targeting the HCV E2 Glycoprotein
title Identification of a Novel Drug Lead That Inhibits HCV Infection and Cell-to-Cell Transmission by Targeting the HCV E2 Glycoprotein
title_full Identification of a Novel Drug Lead That Inhibits HCV Infection and Cell-to-Cell Transmission by Targeting the HCV E2 Glycoprotein
title_fullStr Identification of a Novel Drug Lead That Inhibits HCV Infection and Cell-to-Cell Transmission by Targeting the HCV E2 Glycoprotein
title_full_unstemmed Identification of a Novel Drug Lead That Inhibits HCV Infection and Cell-to-Cell Transmission by Targeting the HCV E2 Glycoprotein
title_short Identification of a Novel Drug Lead That Inhibits HCV Infection and Cell-to-Cell Transmission by Targeting the HCV E2 Glycoprotein
title_sort identification of a novel drug lead that inhibits hcv infection and cell-to-cell transmission by targeting the hcv e2 glycoprotein
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4214736/
https://www.ncbi.nlm.nih.gov/pubmed/25357246
http://dx.doi.org/10.1371/journal.pone.0111333
work_keys_str_mv AT alolabyreemr identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT cocquerellaurence identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT zemlaadam identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT saaslaure identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT dubuissonjean identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT vielmetterjost identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT marcotrigianojoseph identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT khanabdulghafoor identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT catalanfelipevences identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT perrymanalexanderl identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT freundlichjoels identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT forlistefano identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT levyshoshana identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT balhornrod identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein
AT azzazyhassanm identificationofanoveldrugleadthatinhibitshcvinfectionandcelltocelltransmissionbytargetingthehcve2glycoprotein

Ejemplares similares