NK and NKT Cell-Independent Contribution of Interleukin-15 to Innate Protection against Mucosal Viral Infection

doi:10.1128/JVI.79.7.4470-4478.2005

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Journal of Virology, April 2005, p. 4470-4478, Vol. 79, No. 7
0022-538X/05/$08.00+0 doi:10.1128/JVI.79.7.4470-4478.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

NK and NKT Cell-Independent Contribution of Interleukin-15 to Innate Protection against Mucosal Viral Infection

Navkiran Gill, Kenneth L. Rosenthal, and Ali A. Ashkar^*

Centre for Gene Therapeutics, Department of Pathology and Molecular Medicine, McMaster University Health Sciences Centre, Hamilton, Ontario, Canada

Received 27 September 2004/ Accepted 21 October 2004

Interleukin-15 (IL-15) is essential for the development, maturation,and function of NK and NKT cells, which are critical componentsof the innate immune defense against viral infections. We recentlyshowed that mice lacking IL-15 and/or NK/NKT cells are significantlymore susceptible to intravaginal (IVAG) herpes simplex virustype 2 (HSV-2) infection than control mice. For this study,we examined whether IL-15 has any direct antiviral activity,independent of NK/NKT cells, in innate protection against HSV-2infection. A sensitive enzyme-linked immunosorbent assay formurine IL-15 was developed and used to show that IVAG HSV-2infection induces IL-15 in vaginal washes. Using immunohistochemistry,we detected IL-15-positive cells in the submucosa and vaginalepithelium following IVAG HSV-2 infection. Local, but not systemic,delivery of murine recombinant IL-15 (mrIL-15) to the genitalmucosae of IL-15^–/– and RAG-2^–/– ${gamma}$ _c^–/–mice, which both lack NK and NKT cells, resulted in significantreductions in HSV-2 titers in genital washes and 60% survivalfollowing IVAG HSV-2 challenge. Furthermore, we showed thatIL-15 is important for CpG oligodeoxynucleotide (ODN)-inducedinnate protection against genital HSV-2 infection. While 100%of CpG ODN-treated RAG2^–/– ${gamma}$ _c^–/– mice,which are capable of producing IL-15 but lack NK/NKT cells,survived an IVAG HSV-2 challenge, only 60% of CpG ODN-treatedIL-15^–/– mice survived, and all of these mice hadsimilar vaginal viral titers to those in control mice by day3 postchallenge. Lastly, a treatment of RAW264.7 cells withmrIL-15 induced the production of tumor necrosis factor alphaand beta interferon (IFN-ß), but not IFN- ${alpha}$ , and significantlyprotected them against HSV-2 infection in vitro. The resultsof these studies indicate that IL-15 can act independently ofNK/NKT cells in mediating the innate defense against viral infection.

* Corresponding author. Mailing address: Centre for Gene Therapeutics, Department of Pathology and Molecular Medicine, McMaster University Health Sciences Centre, Hamilton, Ontario, Canada L8N 3Z5. Phone: (905) 525-9140, ext. 22311. Fax: (905) 522-6750. E-mail: ashkara{at}mcmaster.ca.

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