Surfactant protein D enhances clearance of influenza A virus from the lung in vivo

AM LeVine, JA Whitsett, KL Hartshorn… - The Journal of …, 2001 - journals.aai.org
AM LeVine, JA Whitsett, KL Hartshorn, EC Crouch, TR Korfhagen
The Journal of Immunology, 2001journals.aai.org
Mice lacking surfactant protein surfactant protein D (SP-D−/−) and wild-type mice (SP-D+/+)
were infected with influenza A virus (IAV) by intranasal instillation. IAV infection increased
the endogenous SP-D concentration in wild-type mice. SP-D-deficient mice showed
decreased viral clearance of the Phil/82 strain of IAV and increased production of
inflammatory cytokines in response to viral challenge. However, the less glycosylated strain
of IAV, Mem/71, which is relatively resistant to SP-D in vitro, was cleared efficiently from the …
Abstract
Mice lacking surfactant protein surfactant protein D (SP-D−/−) and wild-type mice (SP-D+/+) were infected with influenza A virus (IAV) by intranasal instillation. IAV infection increased the endogenous SP-D concentration in wild-type mice. SP-D-deficient mice showed decreased viral clearance of the Phil/82 strain of IAV and increased production of inflammatory cytokines in response to viral challenge. However, the less glycosylated strain of IAV, Mem/71, which is relatively resistant to SP-D in vitro, was cleared efficiently from the lungs of SP-D−/− mice. Viral clearance of the Phil/82 strain of IAV and the cytokine response were both normalized by the coadministration of recombinant SP-D. Since the airway is the usual portal of entry for influenza A virus and other respiratory pathogens, SP-D is likely to play an important role in innate defense responses to IAV.
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