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Antiviral activity of transiently expressed IFN-kappa is cell-associated. | LitMetric

AI Article Synopsis

  • Type I interferons (IFNs) are typically produced by many cell types during viral infections, while IFN-kappa is mainly found in keratinocytes and specific lymphoid cells, demonstrating weaker antiviral activity compared to IFN-beta.
  • To better understand IFN-kappa's antiviral potential, researchers used human cell lines to express IFN-kappa and compared its effects with IFN-alpha2b, discovering that both had similar transcriptional and antiviral activities.
  • However, IFN-kappa's antiviral effects were only detectable in the cells themselves, not in the surrounding culture medium, indicating a unique mechanism of action that could be useful for targeting viral infections, such as hepatitis C.

Article Abstract

Most type I interferons (IFNs) are expressed by the majority of cell types in response to viral infection. In contrast, IFN-kappa has been reported to have a cellular distribution limited to keratinocytes and certain lymphoid cell populations. Recombinant expressed IFN-kappa has been shown previously to possess weak antiviral activity when directly compared with IFN-beta. In order to expand on the antiviral potential of IFN-kappa, we transiently transfected human cell lines to circumvent the need to purify recombinant proteins and to avoid the possible loss of biologic activity by the purification process. We evaluated the transcriptional signaling and antiviral activity of IFN-kappa in parallel with IFN-alpha2b with mammalian expression vectors to express each protein transiently. Both IFN-kappa and IFN-alpha2b exhibited comparable transcriptional and antiviral activities. However, in contrast to IFN-alpha2b transcriptional signaling and antiviral activity, IFN-kappa activity was not detectable in conditioned cell culture medium. Subsequent experiments revealed there was a direct relationship between IFN-kappa-expressing cells and antiviral activity. These results were confirmed in immunocytochemical studies. Furthermore, IFN-kappa exhibited cell-associated antiviral activity against a hepatitis C virus (HCV) replicon cell line. This novel IFN signaling strategy may represent an important distinct and divergent mechanism for limiting viral infections.

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Source
http://dx.doi.org/10.1089/jir.2006.26.40DOI Listing

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