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Protective Role of Beta Interferon in Host Defense Against Influenza A Virus.

Authors:
  • Koerner Iris
  • Kochs Georg
  • Kalinke Ulrich
  • Weiss Siegfried
  • Staeheli Peter

From: Department of Virology, University of Freiburg, Hermann-Herder-Strasse 11, D-79104 Freiburg, Germany.

Journal of virology

  • Publish Date: Feb 2007
  • ISSN: 0022-538X
  • Volume: 81
  • Issue: 4
  • Pages: 2025-30
  • Medium: Print
  • Language: English
  • Citation (JAMA): Koerner Iris, Kochs Georg, Kalinke Ulrich, et al. Protective Role of Beta Interferon in Host Defense Against Influenza A Virus.. J. Virol. Feb 2007;81:2025-30

Abstract

Type I interferon (IFN), which includes the IFN-alpha and -beta subtypes, plays an essential role in host defense against influenza A virus. However, the relative contribution of IFN-beta remains unresolved. In mice, type I IFN is effective against influenza viruses only if the IFN-induced resistance factor Mx1 is present, though most inbred mouse strains, including the recently developed IFN-beta-deficient mice, bear only defective Mx1 alleles. We therefore generated IFN-beta-deficient mice carrying functional Mx1 alleles (designated Mx-BKO) and compared them to either wild-type mice bearing functional copies of both IFN-beta and Mx1 (designated Mx-wt) or mice carrying functional Mx1 alleles but lacking functional type I IFN receptors (designated Mx-IFNAR). Influenza A virus strain SC35M (H7N7) grew to high titers and readily formed plaques in monolayers of Mx-BKO and Mx-IFNAR embryo fibroblasts which showed no spontaneous expression of Mx1. In contrast, Mx-wt embryo fibroblasts were found to constitutively express Mx1, most likely explaining why SC35M did not grow to high titers and formed no visible plaques in such cells. In vivo challenge experiments in which SC35M was applied via the intranasal route showed that the 50% lethal dose was about 20-fold lower in Mx-BKO mice than in Mx-wt mice and that virus titers in the lungs were increased in Mx-BKO mice. The resistance of Mx-BKO mice to influenza A virus strain PR/8/34 (H1N1) was also substantially reduced, demonstrating that IFN-beta plays an important role in the defense against influenza A virus that cannot be compensated for by IFN-alpha.

Mesh Headings (Keywords): Animals, Animals, Genetically Modified, Cells, Cultured, Influenza A Virus, H7N7 Subtype, Interferon-beta, Mice, Mice, Inbred C57BL, Mice, Knockout, Orthomyxoviridae Infections, Receptor, Interferon alpha-beta, Species Specificity

Check for Full Text / PubMed Unique Identifier (PMID): 17151098

This abstract is part of PubMed, a service of the U.S. National Library of Medicine. PubMed includes more than 17 million citations from MEDLINE and other life science journals for biomedical articles. See Copyright and Disclaimers.

Linked medical terms appearing on this page are added by Healia to help readers find more information and are not part of the original PubMed document.

The data herein was last updated on July 8th, 2008 and may not reflect the most current and accurate data available from NLM.

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