TIM-1 Augments Cellular Entry of Ebola Virus Species and Mutants, Which Is Blocked by Recombinant TIM-1 Protein

Ebola virus, a member of the Filoviridae family, utilizes the attachment factors on host cells to support its entry and cause severe tissue damage. TIM-1 has been identified as a predominant attachment factor via interaction with phosphatidylserine (PS) localized on the viral envelope and glycoprote...

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Autores principales: Zhang, Min, Wang, Xinwei, Hu, Linhan, Zhang, Yuting, Zheng, Hang, Wu, Haiyan, Wang, Jing, Luo, Longlong, Xiao, He, Qiao, Chunxia, Li, Xinying, Huang, Weijin, Wang, Youchun, Feng, Jiannan, Chen, Guojiang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9241846/
https://www.ncbi.nlm.nih.gov/pubmed/35384693
http://dx.doi.org/10.1128/spectrum.02212-21
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author Zhang, Min
Wang, Xinwei
Hu, Linhan
Zhang, Yuting
Zheng, Hang
Wu, Haiyan
Wang, Jing
Luo, Longlong
Xiao, He
Qiao, Chunxia
Li, Xinying
Huang, Weijin
Wang, Youchun
Feng, Jiannan
Chen, Guojiang
author_facet Zhang, Min
Wang, Xinwei
Hu, Linhan
Zhang, Yuting
Zheng, Hang
Wu, Haiyan
Wang, Jing
Luo, Longlong
Xiao, He
Qiao, Chunxia
Li, Xinying
Huang, Weijin
Wang, Youchun
Feng, Jiannan
Chen, Guojiang
author_sort Zhang, Min
collection PubMed
description Ebola virus, a member of the Filoviridae family, utilizes the attachment factors on host cells to support its entry and cause severe tissue damage. TIM-1 has been identified as a predominant attachment factor via interaction with phosphatidylserine (PS) localized on the viral envelope and glycoprotein (GP). In this study, we give the first demonstration that TIM-1 enhances the cellular entry of three species of Ebola virus, as well as those harboring GP mutations (A82V, T544I, and A82V T544I). Furthermore, two TIM-1 variants (i.e., TIM-1-359aa and TIM-1-364aa) had comparable effects on promoting Zaire Ebola virus (EBOV) attachment, internalization, and infection. Importantly, recombinant TIM-1 ectodomain (ECD) protein could decrease the infectivity of Ebola virus and display synergistic inhibitory effects with ADI-15946, a monoclonal antibody with broad neutralizing activity to Ebola virus. Of note, EBOV strains harboring GP mutations (K510E and D552N), which were refractory to antibody treatment, were still sensitive to TIM-1 protein-mediated impairment of infectivity, indicating that TIM-1 protein may represent an alternative therapeutic regimen when antibody evasion occurs. IMPORTANCE The viral genome has acquired numerous mutations with the potential to increase transmission during the 2013-to-2016 outbreak of Ebola virus. EBOV strains harboring GP mutations (A82V, T544I, and A82V T544I), which have been identified to increase viral infectivity in humans, have attracted our attention. Herein, we give the first report that polymorphic TIM-1 enhances the infectivity of three species of Ebola virus, as well as those harboring GP mutations (A82V, T544I, and A82V T544I). We show that recombinant TIM-1 ECD protein could decrease the infectivity of Ebola virus with or without a point mutation and displays synergistic inhibitory effects with ADI-15946. Furthermore, TIM-1 protein potently blocked cell entry of antibody-evading Ebola virus species. These findings highlight the role of TIM-1 in Ebola virus infection and indicate that TIM-1 protein represents a potential therapeutic avenue for Ebola virus and its mutated species.
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spelling pubmed-92418462022-06-30 TIM-1 Augments Cellular Entry of Ebola Virus Species and Mutants, Which Is Blocked by Recombinant TIM-1 Protein Zhang, Min Wang, Xinwei Hu, Linhan Zhang, Yuting Zheng, Hang Wu, Haiyan Wang, Jing Luo, Longlong Xiao, He Qiao, Chunxia Li, Xinying Huang, Weijin Wang, Youchun Feng, Jiannan Chen, Guojiang Microbiol Spectr Research Article Ebola virus, a member of the Filoviridae family, utilizes the attachment factors on host cells to support its entry and cause severe tissue damage. TIM-1 has been identified as a predominant attachment factor via interaction with phosphatidylserine (PS) localized on the viral envelope and glycoprotein (GP). In this study, we give the first demonstration that TIM-1 enhances the cellular entry of three species of Ebola virus, as well as those harboring GP mutations (A82V, T544I, and A82V T544I). Furthermore, two TIM-1 variants (i.e., TIM-1-359aa and TIM-1-364aa) had comparable effects on promoting Zaire Ebola virus (EBOV) attachment, internalization, and infection. Importantly, recombinant TIM-1 ectodomain (ECD) protein could decrease the infectivity of Ebola virus and display synergistic inhibitory effects with ADI-15946, a monoclonal antibody with broad neutralizing activity to Ebola virus. Of note, EBOV strains harboring GP mutations (K510E and D552N), which were refractory to antibody treatment, were still sensitive to TIM-1 protein-mediated impairment of infectivity, indicating that TIM-1 protein may represent an alternative therapeutic regimen when antibody evasion occurs. IMPORTANCE The viral genome has acquired numerous mutations with the potential to increase transmission during the 2013-to-2016 outbreak of Ebola virus. EBOV strains harboring GP mutations (A82V, T544I, and A82V T544I), which have been identified to increase viral infectivity in humans, have attracted our attention. Herein, we give the first report that polymorphic TIM-1 enhances the infectivity of three species of Ebola virus, as well as those harboring GP mutations (A82V, T544I, and A82V T544I). We show that recombinant TIM-1 ECD protein could decrease the infectivity of Ebola virus with or without a point mutation and displays synergistic inhibitory effects with ADI-15946. Furthermore, TIM-1 protein potently blocked cell entry of antibody-evading Ebola virus species. These findings highlight the role of TIM-1 in Ebola virus infection and indicate that TIM-1 protein represents a potential therapeutic avenue for Ebola virus and its mutated species. American Society for Microbiology 2022-04-06 /pmc/articles/PMC9241846/ /pubmed/35384693 http://dx.doi.org/10.1128/spectrum.02212-21 Text en Copyright © 2022 Zhang et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Zhang, Min
Wang, Xinwei
Hu, Linhan
Zhang, Yuting
Zheng, Hang
Wu, Haiyan
Wang, Jing
Luo, Longlong
Xiao, He
Qiao, Chunxia
Li, Xinying
Huang, Weijin
Wang, Youchun
Feng, Jiannan
Chen, Guojiang
TIM-1 Augments Cellular Entry of Ebola Virus Species and Mutants, Which Is Blocked by Recombinant TIM-1 Protein
title TIM-1 Augments Cellular Entry of Ebola Virus Species and Mutants, Which Is Blocked by Recombinant TIM-1 Protein
title_full TIM-1 Augments Cellular Entry of Ebola Virus Species and Mutants, Which Is Blocked by Recombinant TIM-1 Protein
title_fullStr TIM-1 Augments Cellular Entry of Ebola Virus Species and Mutants, Which Is Blocked by Recombinant TIM-1 Protein
title_full_unstemmed TIM-1 Augments Cellular Entry of Ebola Virus Species and Mutants, Which Is Blocked by Recombinant TIM-1 Protein
title_short TIM-1 Augments Cellular Entry of Ebola Virus Species and Mutants, Which Is Blocked by Recombinant TIM-1 Protein
title_sort tim-1 augments cellular entry of ebola virus species and mutants, which is blocked by recombinant tim-1 protein
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9241846/
https://www.ncbi.nlm.nih.gov/pubmed/35384693
http://dx.doi.org/10.1128/spectrum.02212-21
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