TTK inhibition radiosensitizes basal-like breast cancer through impaired homologous recombination
Benjamin C. Chandler, … , Arul Chinnaiyan, Corey Speers
Benjamin C. Chandler, … , Arul Chinnaiyan, Corey Speers
Published January 21, 2020
Citation Information: J Clin Invest. 2020;130(2):958-973. https://doi.org/10.1172/JCI130435.
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Research Article Oncology

TTK inhibition radiosensitizes basal-like breast cancer through impaired homologous recombination

Abstract

Increased rates of locoregional recurrence are observed in patients with basal-like breast cancer (BC) despite the use of radiation therapy (RT); therefore, approaches that result in radiosensitization of basal-like BC are critically needed. Using patients’ tumor gene expression data from 4 independent data sets, we correlated gene expression with recurrence to find genes significantly correlated with early recurrence after RT. The highest-ranked gene, TTK, was most highly expressed in basal-like BC across multiple data sets. Inhibition of TTK by both genetic and pharmacologic methods enhanced radiosensitivity in multiple basal-like cell lines. Radiosensitivity was mediated, at least in part, through persistent DNA damage after treatment with TTK inhibition and RT. Inhibition of TTK impaired homologous recombination (HR) and repair efficiency, but not nonhomologous end-joining, and decreased the formation of Rad51 foci. Reintroduction of wild-type TTK rescued both radioresistance and HR repair efficiency after TTK knockdown; however, reintroduction of kinase-dead TTK did not. In vivo, TTK inhibition combined with RT led to a significant decrease in tumor growth in both heterotopic and orthotopic, including patient-derived xenograft, BC models. These data support the rationale for clinical development of TTK inhibition as a radiosensitizing strategy for patients with basal-like BC, and efforts toward this end are currently underway.

Authors

Benjamin C. Chandler, Leah Moubadder, Cassandra L. Ritter, Meilan Liu, Meleah Cameron, Kari Wilder-Romans, Amanda Zhang, Andrea M. Pesch, Anna R. Michmerhuizen, Nicole Hirsh, Marlie Androsiglio, Tanner Ward, Eric Olsen, Yashar S. Niknafs, Sofia Merajver, Dafydd G. Thomas, Powel H. Brown, Theodore S. Lawrence, Shyam Nyati, Lori J. Pierce, Arul Chinnaiyan, Corey Speers

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Figure 3

TTK inhibition in combination with RT leads to persistent dsDNA damage over time.

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TTK inhibition in combination with RT leads to persistent dsDNA damage o...
(A and B) Combination treatment of Dox-inducible shRNA and RT led to persistent dsDNA damage over time in 2 basal-like BC cell lines: MDA-MB-231 (A) and BT-549 (B). (C) Representative images of BT-549 γH2AX foci at 16 hours. Original magnification, ×60. (D and E) Pharmacological inhibition of TTK kinase function, using B909, in combination with RT led to persistent dsDNA damage over time in 2 basal-like BC cell lines, MDA-MB-231 (D) and BT-549 (E). (F) Representative images of MDA-MB-231 γH2AX foci at 24 hours. Original magnification, ×60. Data represent the mean of 3 independent experiments repeated in triplicate, with approximately 100 cells counted for each experiment, and error bars represent SD. A 2-sided Student’s t test was used for comparison. *P < 0.05 and **P < 0.01