TTK inhibitor OSU13 promotes immunotherapy responses by activating tumor STING
Vijaya Bharti, Amrendra Kumar, Yinchong Wang, Nikhil Roychowdhury, Daniel de Lima Bellan, Beimnet B. Kassaye, Reese Watkins, Marina Capece, Catherine G. Chung, Gerard Hilinski, Anna E. Vilgelm
Vijaya Bharti, Amrendra Kumar, Yinchong Wang, Nikhil Roychowdhury, Daniel de Lima Bellan, Beimnet B. Kassaye, Reese Watkins, Marina Capece, Catherine G. Chung, Gerard Hilinski, Anna E. Vilgelm
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Research Article Oncology

TTK inhibitor OSU13 promotes immunotherapy responses by activating tumor STING

Abstract

TTK spindle assembly checkpoint kinase is an emerging cancer target. This preclinical study explored the antitumor mechanism of TTK inhibitor OSU13 to define a strategy for clinical development. We observed prominent antitumor activity of OSU13 in melanoma, colon and breast cancer cells, organoids derived from patients with melanoma, and mice bearing colon tumors associated with G2 cell cycle arrest, senescence, and apoptosis. OSU13-treated cells displayed DNA damage and micronuclei that triggered the cytosolic DNA-sensing cGAS/STING pathway. STING was required for the induction of several proteins involved in T cell recruitment and activity. Tumors from OSU13-treated mice showed an increased proportion of T and NK cells and evidence of PD-1/PD-L1 immune checkpoint activation. Combining a low-toxicity dose of OSU13 with anti–PD-1 checkpoint blockade resulted in prominent STING- and CD8+ T cell–dependent tumor inhibition and improved survival. These findings provide a rationale for utilizing TTK inhibitors in combination with immunotherapy in STING-proficient tumors.

Authors

Vijaya Bharti, Amrendra Kumar, Yinchong Wang, Nikhil Roychowdhury, Daniel de Lima Bellan, Beimnet B. Kassaye, Reese Watkins, Marina Capece, Catherine G. Chung, Gerard Hilinski, Anna E. Vilgelm

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Figure 6

OSU13 augments immunotherapy responses in mice.

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OSU13 augments immunotherapy responses in mice. Growth of MC38 tumors tr...
Growth of MC38 tumors treated with vehicle or OSU13 (10 mg/kg, 5 days a week) in the absence or presence of 100 μg anti–PD-1 or isotype antibody treatment (dose). N = 6–10 mice per group. Statistics using a mixed model with Tukey’s post test. (B) Survival of mice shown in A. Statistical comparison between vehicle and OSU13 and anti–PD-1 combination group is indicated. (C) Results of the tumor rechallenge experiment. MC38 tumor cells were injected in 4 mice that rejected tumors after OSU13 and anti–PD-1–treatment (from experiment in A) and in 6 tumor-naive mice. Rechallenge was performed 2 months after therapy completion. Areas in blue indicate mice that did not develop tumors. (D) MC38 tumor growth in CD8+ T cell–depleted and nondepleted mice treated with OSU13 and anti–PD-1. N = 8 mice per group. Statistics using mixed model. (E) Response of WT and STING-KO tumors to OSU13 and anti–PD-1 combination treatment. N = 9–11 mice per group. Statistics using mixed model. **P < 0.01; ****P < 0.0001.