Interferon alpha bioactivity critically depends on Scavenger receptor class B type I function

نویسندگان

  • Marcos Vasquez
  • Jessica Fioravanti
  • Fernando Aranda
  • Vladimir Paredes
  • Celia Gomar
  • Nuria Ardaiz
  • Veronica Fernandez-Ruiz
  • Miriam Méndez
  • Estanislao Nistal-Villan
  • Esther Larrea
  • Qinshan Gao
  • Gloria Gonzalez-Aseguinolaza
  • Jesus Prieto
  • Pedro Berraondo
چکیده

Scavenger receptor class B type I (SR-B1) binds pathogen-associated molecular patterns participating in the regulation of the inflammatory reaction but there is no information regarding potential interactions between SR-B1 and the interferon system. Herein, we report that SR-B1 ligands strongly regulate the transcriptional response to interferon α (IFNα) and enhance its antiviral and antitumor activity. This effect was mediated by the activation of TLR2 and TLR4 as it was annulled by the addition of anti-TLR2 or anti-TLR4 blocking antibodies. In vivo, we maximized the antitumor activity of IFNα co-expressing in the liver a SR-B1 ligand and IFNα by adeno-associated viruses. This gene therapy strategy eradicated liver metastases from colon cancer with reduced toxicity. On the other hand, genetic and pharmacological inhibition of SR-B1 blocks the clathrin-dependent interferon receptor recycling pathway with a concomitant reduction in IFNα signaling and bioactivity. This effect can be applied to enhance cancer immunotherapy with oncolytic viruses. Indeed, SR-B1 antagonists facilitate replication of oncolytic viruses amplifying their tumoricidal potential. In conclusion, SR-B1 agonists behave as IFNα enhancers while SR-B1 inhibitors dampen IFNα activity. These results demonstrate that SR-B1 is a suitable pharmacology target to enhance cancer immunotherapy based on IFNα and oncolytic viruses.

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عنوان ژورنال:

دوره 5  شماره 

صفحات  -

تاریخ انتشار 2016