Cytokine therapy reverses NK cell anergy in MHC-deficient tumors
Michele Ardolino, … , K. Christopher Garcia, David H. Raulet
Michele Ardolino, … , K. Christopher Garcia, David H. Raulet
Published October 20, 2014
Citation Information: J Clin Invest. 2014;124(11):4781-4794. https://doi.org/10.1172/JCI74337.
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Research Article

Cytokine therapy reverses NK cell anergy in MHC-deficient tumors

Abstract

Various cytokines have been evaluated as potential anticancer drugs; however, most cytokine trials have shown relatively low efficacy. Here, we found that treatments with IL-12 and IL-18 or with a mutant form of IL-2 (the “superkine” called H9) provided substantial therapeutic benefit for mice specifically bearing MHC class I–deficient tumors, but these treatments were ineffective for mice with matched MHC class I+ tumors. Cytokine efficacy was linked to the reversal of the anergic state of NK cells that specifically occurred in MHC class I–deficient tumors, but not MHC class I+ tumors. NK cell anergy was accompanied by impaired early signal transduction and was locally imparted by the presence of MHC class I–deficient tumor cells, even when such cells were a minor population in a tumor mixture. These results demonstrate that MHC class I–deficient tumor cells can escape from the immune response by functionally inactivating NK cells, and suggest cytokine-based immunotherapy as a potential strategy for MHC class I–deficient tumors. These results suggest that such cytokine therapies would be optimized by stratification of patients. Moreover, our results suggest that such treatments may be highly beneficial in the context of therapies to enhance NK cell functions in cancer patients.

Authors

Michele Ardolino, Camillia S. Azimi, Alexandre Iannello, Troy N. Trevino, Lucas Horan, Lily Zhang, Weiwen Deng, Aaron M. Ring, Suzanne Fischer, K. Christopher Garcia, David H. Raulet

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Figure 4

Anergy of NK cells infiltrating MHC class I–deficient mutants of the C1498 cell line.

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Anergy of NK cells infiltrating MHC class I–deficient mutants of the C14...
C1498, C1498-B2m, and C1498-Tap2 cells were implanted s.c. into B6 mice. After 14 days, tumor volume was measured (A), and NK cell infiltration (B) and responsiveness (C) were assessed as described in the legend to Figure 3. In C, 2 independent experiments are shown. Bars represent means ± SD. NK cells were gated as in Figure 3. The experiments included at least 5 mice per group. Statistical analyses were performed with the 2-tailed unpaired Student’s t test.