OncoImmunology (Jan 2018)

Sunitinib represses regulatory T cells to overcome immunotolerance in a murine model of hepatocellular cancer

  • Dai Liu,
  • Guangfu Li,
  • Diego M. Avella,
  • Eric T. Kimchi,
  • Jussuf T. Kaifi,
  • Mark P. Rubinstein,
  • E. Ramsay Camp,
  • Don C. Rockey,
  • Todd D. Schell,
  • Kevin F. Staveley-O'Carroll

DOI
https://doi.org/10.1080/2162402X.2017.1372079
Journal volume & issue
Vol. 7, no. 1

Abstract

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Successful development of immunotherapeutic strategies for hepatocellular cancer (HCC) has been impeded by limited understanding of tumor-induced profound tolerance and lack of a clinically faithful HCC model. Recently, we developed a novel model that recapitulates typical features of human HCC. Using this clinically relevant model, we demonstrate that tumor growth impairs host immunity and causes a profound exhaustion of tumor antigen-specific (TAS) CD8+ T cells. Increase in frequency and suppressive function of regulatory T cells (Tregs) is critically involved in this tumor-induced immune dysfunction. We further demonstrate that sunitinib suppresses Tregs and prevents tumor-induced immune tolerance, allowing TAS immunization to activate endogenous CD8+ T cells. As a result, this combinational strategy delays tumor growth. Importantly, the additional integration of exogenous naïve TAS CD8+ T cells by adoptive cell transfer (ACT) leads to the elimination of the established tumors without recurrence and promotes long-term survival of the treated mice. Mechanistically, sunitinib treatment primes the antitumor immune response by significantly decreasing Treg frequency, reducing TGF-β and IL-10 production by Tregs, and also protecting TAS CD8+ T cells from tumor-induced deletion in the setting of HCC. Taken together, sunitinib quantitatively and qualitatively modifies Tregs to overcome tumor-induced immune deficiency, suggesting the potential of sunitinib as a therapeutic immune activator for HCC control.

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