Novel strategies for targeting innate immune responses to influenza.

K.A. Shirey; W. Lai; M.C. Patel; L.M. Pletneva; C. Pang; E. Kurt-Jones; M. Lipsky; T. Roger; T. Calandra; K.J. Tracey; Y. Al-Abed; A.G. Bowie; A. Fasano; C.A. Dinarello; F. Gusovsky; J.C. Blanco; S.N. Vogel

Novel strategies for targeting innate immune responses to influenza.

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Anglais

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doi: 10.1038/mi.2015.141
issn: 1933-0219

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Serveur académique Lausannois

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Ce document est lié à :
info:eu-repo/semantics/altIdentifier/doi/10.1038/mi.2015.141

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info:eu-repo/semantics/altIdentifier/pmid/26813341

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info:eu-repo/semantics/altIdentifier/eissn/1935-3456

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info:eu-repo/semantics/altIdentifier/urn/urn:nbn:ch:serval-BIB_0694E43E48275

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Serveur Académique Lausannois

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Université de Lausanne et CHUV

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info:eu-repo/semantics/openAccess , Copying allowed only for non-profit organizations , https://serval.unil.ch/disclaimer

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Infectious diseases

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K.A. Shirey et al., « Novel strategies for targeting innate immune responses to influenza. », Serveur académique Lausannois, ID : 10.1038/mi.2015.141

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We previously reported that TLR4(-/-) mice are refractory to mouse-adapted A/PR/8/34 (PR8) influenza-induced lethality and that therapeutic administration of the TLR4 antagonist Eritoran blocked PR8-induced lethality and acute lung injury (ALI) when given starting 2 days post infection. Herein we extend these findings: anti-TLR4- or -TLR2-specific IgG therapy also conferred significant protection of wild-type (WT) mice from lethal PR8 infection. If treatment is initiated 3 h before PR8 infection and continued daily for 4 days, Eritoran failed to protect WT and TLR4(-/-) mice, implying that Eritoran must block a virus-induced, non-TLR4 signal that is required for protection. Mechanistically, we determined that (i) Eritoran blocks high-mobility group B1 (HMGB1)-mediated, TLR4-dependent signaling in vitro and circulating HMGB1 in vivo, and an HMGB1 inhibitor protects against PR8; (ii) Eritoran inhibits pulmonary lung edema associated with ALI; (iii) interleukin (IL)-1β contributes significantly to PR8-induced lethality, as evidenced by partial protection by IL-1 receptor antagonist (IL-1Ra) therapy. Synergistic protection against PR8-induced lethality was achieved when Eritoran and the antiviral drug oseltamivir were administered starting 4 days post infection. Eritoran treatment does not prevent development of an adaptive immune response to subsequent PR8 challenge. Overall, our data support the potential of a host-targeted therapeutic approach to influenza infection.

Novel strategies for targeting innate immune responses to influenza.

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