Lectin-Dependent Enhancement of Ebola Virus Infection via Soluble and Transmembrane C-type Lectin Receptors

Mannose-binding lectin (MBL) is a key soluble effector of the innate immune system that recognizes pathogen-specific surface glycans. Surprisingly, low-producing MBL genetic variants that may predispose children and immunocompromised individuals to infectious diseases are more common than would be e...

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Autores principales: Brudner, Matthew, Karpel, Marshall, Lear, Calli, Chen, Li, Yantosca, L. Michael, Scully, Corinne, Sarraju, Ashish, Sokolovska, Anna, Zariffard, M. Reza, Eisen, Damon P., Mungall, Bruce A., Kotton, Darrell N., Omari, Amel, Huang, I-Chueh, Farzan, Michael, Takahashi, Kazue, Stuart, Lynda, Stahl, Gregory L., Ezekowitz, Alan B., Spear, Gregory T., Olinger, Gene G., Schmidt, Emmett V., Michelow, Ian C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3614905/
https://www.ncbi.nlm.nih.gov/pubmed/23573288
http://dx.doi.org/10.1371/journal.pone.0060838
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author Brudner, Matthew
Karpel, Marshall
Lear, Calli
Chen, Li
Yantosca, L. Michael
Scully, Corinne
Sarraju, Ashish
Sokolovska, Anna
Zariffard, M. Reza
Eisen, Damon P.
Mungall, Bruce A.
Kotton, Darrell N.
Omari, Amel
Huang, I-Chueh
Farzan, Michael
Takahashi, Kazue
Stuart, Lynda
Stahl, Gregory L.
Ezekowitz, Alan B.
Spear, Gregory T.
Olinger, Gene G.
Schmidt, Emmett V.
Michelow, Ian C.
author_facet Brudner, Matthew
Karpel, Marshall
Lear, Calli
Chen, Li
Yantosca, L. Michael
Scully, Corinne
Sarraju, Ashish
Sokolovska, Anna
Zariffard, M. Reza
Eisen, Damon P.
Mungall, Bruce A.
Kotton, Darrell N.
Omari, Amel
Huang, I-Chueh
Farzan, Michael
Takahashi, Kazue
Stuart, Lynda
Stahl, Gregory L.
Ezekowitz, Alan B.
Spear, Gregory T.
Olinger, Gene G.
Schmidt, Emmett V.
Michelow, Ian C.
author_sort Brudner, Matthew
collection PubMed
description Mannose-binding lectin (MBL) is a key soluble effector of the innate immune system that recognizes pathogen-specific surface glycans. Surprisingly, low-producing MBL genetic variants that may predispose children and immunocompromised individuals to infectious diseases are more common than would be expected in human populations. Since certain immune defense molecules, such as immunoglobulins, can be exploited by invasive pathogens, we hypothesized that MBL might also enhance infections in some circumstances. Consequently, the low and intermediate MBL levels commonly found in human populations might be the result of balancing selection. Using model infection systems with pseudotyped and authentic glycosylated viruses, we demonstrated that MBL indeed enhances infection of Ebola, Hendra, Nipah and West Nile viruses in low complement conditions. Mechanistic studies with Ebola virus (EBOV) glycoprotein pseudotyped lentiviruses confirmed that MBL binds to N-linked glycan epitopes on viral surfaces in a specific manner via the MBL carbohydrate recognition domain, which is necessary for enhanced infection. MBL mediates lipid-raft-dependent macropinocytosis of EBOV via a pathway that appears to require less actin or early endosomal processing compared with the filovirus canonical endocytic pathway. Using a validated RNA interference screen, we identified C1QBP (gC1qR) as a candidate surface receptor that mediates MBL-dependent enhancement of EBOV infection. We also identified dectin-2 (CLEC6A) as a potentially novel candidate attachment factor for EBOV. Our findings support the concept of an innate immune haplotype that represents critical interactions between MBL and complement component C4 genes and that may modify susceptibility or resistance to certain glycosylated pathogens. Therefore, higher levels of native or exogenous MBL could be deleterious in the setting of relative hypocomplementemia which can occur genetically or because of immunodepletion during active infections. Our findings confirm our hypothesis that the pressure of infectious diseases may have contributed in part to evolutionary selection of MBL mutant haplotypes.
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spelling pubmed-36149052013-04-09 Lectin-Dependent Enhancement of Ebola Virus Infection via Soluble and Transmembrane C-type Lectin Receptors Brudner, Matthew Karpel, Marshall Lear, Calli Chen, Li Yantosca, L. Michael Scully, Corinne Sarraju, Ashish Sokolovska, Anna Zariffard, M. Reza Eisen, Damon P. Mungall, Bruce A. Kotton, Darrell N. Omari, Amel Huang, I-Chueh Farzan, Michael Takahashi, Kazue Stuart, Lynda Stahl, Gregory L. Ezekowitz, Alan B. Spear, Gregory T. Olinger, Gene G. Schmidt, Emmett V. Michelow, Ian C. PLoS One Research Article Mannose-binding lectin (MBL) is a key soluble effector of the innate immune system that recognizes pathogen-specific surface glycans. Surprisingly, low-producing MBL genetic variants that may predispose children and immunocompromised individuals to infectious diseases are more common than would be expected in human populations. Since certain immune defense molecules, such as immunoglobulins, can be exploited by invasive pathogens, we hypothesized that MBL might also enhance infections in some circumstances. Consequently, the low and intermediate MBL levels commonly found in human populations might be the result of balancing selection. Using model infection systems with pseudotyped and authentic glycosylated viruses, we demonstrated that MBL indeed enhances infection of Ebola, Hendra, Nipah and West Nile viruses in low complement conditions. Mechanistic studies with Ebola virus (EBOV) glycoprotein pseudotyped lentiviruses confirmed that MBL binds to N-linked glycan epitopes on viral surfaces in a specific manner via the MBL carbohydrate recognition domain, which is necessary for enhanced infection. MBL mediates lipid-raft-dependent macropinocytosis of EBOV via a pathway that appears to require less actin or early endosomal processing compared with the filovirus canonical endocytic pathway. Using a validated RNA interference screen, we identified C1QBP (gC1qR) as a candidate surface receptor that mediates MBL-dependent enhancement of EBOV infection. We also identified dectin-2 (CLEC6A) as a potentially novel candidate attachment factor for EBOV. Our findings support the concept of an innate immune haplotype that represents critical interactions between MBL and complement component C4 genes and that may modify susceptibility or resistance to certain glycosylated pathogens. Therefore, higher levels of native or exogenous MBL could be deleterious in the setting of relative hypocomplementemia which can occur genetically or because of immunodepletion during active infections. Our findings confirm our hypothesis that the pressure of infectious diseases may have contributed in part to evolutionary selection of MBL mutant haplotypes. Public Library of Science 2013-04-02 /pmc/articles/PMC3614905/ /pubmed/23573288 http://dx.doi.org/10.1371/journal.pone.0060838 Text en © 2013 Brudner 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
Brudner, Matthew
Karpel, Marshall
Lear, Calli
Chen, Li
Yantosca, L. Michael
Scully, Corinne
Sarraju, Ashish
Sokolovska, Anna
Zariffard, M. Reza
Eisen, Damon P.
Mungall, Bruce A.
Kotton, Darrell N.
Omari, Amel
Huang, I-Chueh
Farzan, Michael
Takahashi, Kazue
Stuart, Lynda
Stahl, Gregory L.
Ezekowitz, Alan B.
Spear, Gregory T.
Olinger, Gene G.
Schmidt, Emmett V.
Michelow, Ian C.
Lectin-Dependent Enhancement of Ebola Virus Infection via Soluble and Transmembrane C-type Lectin Receptors
title Lectin-Dependent Enhancement of Ebola Virus Infection via Soluble and Transmembrane C-type Lectin Receptors
title_full Lectin-Dependent Enhancement of Ebola Virus Infection via Soluble and Transmembrane C-type Lectin Receptors
title_fullStr Lectin-Dependent Enhancement of Ebola Virus Infection via Soluble and Transmembrane C-type Lectin Receptors
title_full_unstemmed Lectin-Dependent Enhancement of Ebola Virus Infection via Soluble and Transmembrane C-type Lectin Receptors
title_short Lectin-Dependent Enhancement of Ebola Virus Infection via Soluble and Transmembrane C-type Lectin Receptors
title_sort lectin-dependent enhancement of ebola virus infection via soluble and transmembrane c-type lectin receptors
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3614905/
https://www.ncbi.nlm.nih.gov/pubmed/23573288
http://dx.doi.org/10.1371/journal.pone.0060838
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