Receptor Complementation and Mutagenesis Reveal SR-BI as an Essential HCV Entry Factor and Functionally Imply Its Intra- and Extra-Cellular Domains

HCV entry into cells is a multi-step and slow process. It is believed that the initial capture of HCV particles by glycosaminoglycans and/or lipoprotein receptors is followed by coordinated interactions with the scavenger receptor class B type I (SR-BI), a major receptor of high-density lipoprotein...

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Autores principales: Dreux, Marlène, Dao Thi, Viet Loan, Fresquet, Judith, Guérin, Maryse, Julia, Zélie, Verney, Géraldine, Durantel, David, Zoulim, Fabien, Lavillette, Dimitri, Cosset, François-Loïc, Bartosch, Birke
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2009
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2636890/
https://www.ncbi.nlm.nih.gov/pubmed/19229312
http://dx.doi.org/10.1371/journal.ppat.1000310
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author Dreux, Marlène
Dao Thi, Viet Loan
Fresquet, Judith
Guérin, Maryse
Julia, Zélie
Verney, Géraldine
Durantel, David
Zoulim, Fabien
Lavillette, Dimitri
Cosset, François-Loïc
Bartosch, Birke
author_facet Dreux, Marlène
Dao Thi, Viet Loan
Fresquet, Judith
Guérin, Maryse
Julia, Zélie
Verney, Géraldine
Durantel, David
Zoulim, Fabien
Lavillette, Dimitri
Cosset, François-Loïc
Bartosch, Birke
author_sort Dreux, Marlène
collection PubMed
description HCV entry into cells is a multi-step and slow process. It is believed that the initial capture of HCV particles by glycosaminoglycans and/or lipoprotein receptors is followed by coordinated interactions with the scavenger receptor class B type I (SR-BI), a major receptor of high-density lipoprotein (HDL), the CD81 tetraspanin, and the tight junction protein Claudin-1, ultimately leading to uptake and cellular penetration of HCV via low-pH endosomes. Several reports have indicated that HDL promotes HCV entry through interaction with SR-BI. This pathway remains largely elusive, although it was shown that HDL neither associates with HCV particles nor modulates HCV binding to SR-BI. In contrast to CD81 and Claudin-1, the importance of SR-BI has only been addressed indirectly because of lack of cells in which functional complementation assays with mutant receptors could be performed. Here we identified for the first time two cell types that supported HCVpp and HCVcc entry upon ectopic SR-BI expression. Remarkably, the undetectable expression of SR-BI in rat hepatoma cells allowed unambiguous investigation of human SR-BI functions during HCV entry. By expressing different SR-BI mutants in either cell line, our results revealed features of SR-BI intracellular domains that influence HCV infectivity without affecting receptor binding and stimulation of HCV entry induced by HDL/SR-BI interaction. Conversely, we identified positions of SR-BI ectodomain that, by altering HCV binding, inhibit entry. Finally, we characterized alternative ectodomain determinants that, by reducing SR-BI cholesterol uptake and efflux functions, abolish HDL-mediated infection-enhancement. Altogether, we demonstrate that SR-BI is an essential HCV entry factor. Moreover, our results highlight specific SR-BI determinants required during HCV entry and physiological lipid transfer functions hijacked by HCV to favor infection.
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spelling pubmed-26368902009-02-20 Receptor Complementation and Mutagenesis Reveal SR-BI as an Essential HCV Entry Factor and Functionally Imply Its Intra- and Extra-Cellular Domains Dreux, Marlène Dao Thi, Viet Loan Fresquet, Judith Guérin, Maryse Julia, Zélie Verney, Géraldine Durantel, David Zoulim, Fabien Lavillette, Dimitri Cosset, François-Loïc Bartosch, Birke PLoS Pathog Research Article HCV entry into cells is a multi-step and slow process. It is believed that the initial capture of HCV particles by glycosaminoglycans and/or lipoprotein receptors is followed by coordinated interactions with the scavenger receptor class B type I (SR-BI), a major receptor of high-density lipoprotein (HDL), the CD81 tetraspanin, and the tight junction protein Claudin-1, ultimately leading to uptake and cellular penetration of HCV via low-pH endosomes. Several reports have indicated that HDL promotes HCV entry through interaction with SR-BI. This pathway remains largely elusive, although it was shown that HDL neither associates with HCV particles nor modulates HCV binding to SR-BI. In contrast to CD81 and Claudin-1, the importance of SR-BI has only been addressed indirectly because of lack of cells in which functional complementation assays with mutant receptors could be performed. Here we identified for the first time two cell types that supported HCVpp and HCVcc entry upon ectopic SR-BI expression. Remarkably, the undetectable expression of SR-BI in rat hepatoma cells allowed unambiguous investigation of human SR-BI functions during HCV entry. By expressing different SR-BI mutants in either cell line, our results revealed features of SR-BI intracellular domains that influence HCV infectivity without affecting receptor binding and stimulation of HCV entry induced by HDL/SR-BI interaction. Conversely, we identified positions of SR-BI ectodomain that, by altering HCV binding, inhibit entry. Finally, we characterized alternative ectodomain determinants that, by reducing SR-BI cholesterol uptake and efflux functions, abolish HDL-mediated infection-enhancement. Altogether, we demonstrate that SR-BI is an essential HCV entry factor. Moreover, our results highlight specific SR-BI determinants required during HCV entry and physiological lipid transfer functions hijacked by HCV to favor infection. Public Library of Science 2009-02-20 /pmc/articles/PMC2636890/ /pubmed/19229312 http://dx.doi.org/10.1371/journal.ppat.1000310 Text en Dreux et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Dreux, Marlène
Dao Thi, Viet Loan
Fresquet, Judith
Guérin, Maryse
Julia, Zélie
Verney, Géraldine
Durantel, David
Zoulim, Fabien
Lavillette, Dimitri
Cosset, François-Loïc
Bartosch, Birke
Receptor Complementation and Mutagenesis Reveal SR-BI as an Essential HCV Entry Factor and Functionally Imply Its Intra- and Extra-Cellular Domains
title Receptor Complementation and Mutagenesis Reveal SR-BI as an Essential HCV Entry Factor and Functionally Imply Its Intra- and Extra-Cellular Domains
title_full Receptor Complementation and Mutagenesis Reveal SR-BI as an Essential HCV Entry Factor and Functionally Imply Its Intra- and Extra-Cellular Domains
title_fullStr Receptor Complementation and Mutagenesis Reveal SR-BI as an Essential HCV Entry Factor and Functionally Imply Its Intra- and Extra-Cellular Domains
title_full_unstemmed Receptor Complementation and Mutagenesis Reveal SR-BI as an Essential HCV Entry Factor and Functionally Imply Its Intra- and Extra-Cellular Domains
title_short Receptor Complementation and Mutagenesis Reveal SR-BI as an Essential HCV Entry Factor and Functionally Imply Its Intra- and Extra-Cellular Domains
title_sort receptor complementation and mutagenesis reveal sr-bi as an essential hcv entry factor and functionally imply its intra- and extra-cellular domains
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2636890/
https://www.ncbi.nlm.nih.gov/pubmed/19229312
http://dx.doi.org/10.1371/journal.ppat.1000310
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