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NKp30-dependent cytolysis of filovirus-infected human dendritic cells.

作者信息

Fuller Claudette L, Ruthel Gordon, Warfield Kelly L, Swenson Dana L, Bosio Catharine M, Aman M Javad, Bavari Sina

机构信息

United States Army Medical Research Institute of Infectious Diseases, Frederick, MD 21702, USA.

出版信息

Cell Microbiol. 2007 Apr;9(4):962-76. doi: 10.1111/j.1462-5822.2006.00844.x.


DOI:10.1111/j.1462-5822.2006.00844.x
PMID:17381429
Abstract

Understanding how protective innate immune responses are generated is crucial to defeating highly lethal emerging pathogens. Accumulating evidence suggests that potent innate immune responses are tightly linked to control of Ebola and Marburg filoviral infections. Here, we report that unlike authentic or inactivated Ebola and Marburg, filovirus-derived virus-like particles directly activated human natural killer (NK) cells in vitro, evidenced by pro-inflammatory cytokine production and enhanced cytolysis of permissive target cells. Further, we observed perforin- and CD95L-mediated cytolysis of filovirus-infected human dendritic cells (DCs), primary targets of filovirus infection, by autologous NK cells. Gene expression knock-down studies directly linked NK cell lysis of infected DCs to upregulation of the natural cytotoxicity receptor, NKp30. These results are the first to propose a role for NK cells in the clearance of infected DCs and the potential involvement of NKp30-mediated cytolysis in control of viral infection in vivo. Further elucidation of the biology of NK cell activation, specifically natural cytotoxicity receptors like NKp30 and NKp46, promises to aid our understanding of microbial pathology.

摘要

相似文献

[1]
NKp30-dependent cytolysis of filovirus-infected human dendritic cells.

Cell Microbiol. 2007-4

[2]
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[3]
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[6]
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[7]
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[9]
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[10]
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[2]
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[3]
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[4]
Filoviruses: Innate Immunity, Inflammatory Cell Death, and Cytokines.

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[5]
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[6]
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[7]
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J Innate Immun. 2022

[8]
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Clin Transl Immunology. 2021-1-18

[9]
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Curr Opin Virol. 2020-10

[10]
Distinct Immunogenicity and Efficacy of Poxvirus-Based Vaccine Candidates against Ebola Virus Expressing GP and VP40 Proteins.

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