https://orcid.org/0000-0002-3756-4227
Abstract
The ataxia telangiectasia mutated (ATM) protein coordinates the cellular response to therapeutic radiation, and ATM inhibitors can potentially enhance the efficacy of radiation in otherwise radiation-resistant tumors.
The small molecule ATM kinase inhibitor WSD0628 was specifically designed for enhanced distribution across the blood brain barrier to more effectively treat glioblastoma (GBM) and brain metastases in combination with radiation therapy (RT). GBM and brain metastasis patient-derived xenograft (PDX) models were used to understand target inhibition, radiosensitization, inhibition of the DNA damage response, and in vivo efficacy.
Initial in vitro characterization of WSD0628 demonstrate a high-level of selectivity across kinase families, limited aldehyde oxidase liability, and low risk of hERG interactions. Consistent with a central role for ATM in radiation response, WSD0628 blocked radiation-induced signaling and enhanced radiosensitivity in U251 glioma cells and brain tumor PDXs GBM120 and M12. In comparison to control or RT alone in orthotopic PDXs, the combination of WSD0628 with RT markedly prolonged median survival – GBM12 (19, 55 and 408 days, respectively); GBM43 (26, 44 and 143 days, respectively); GBM120 (51, 89 and 231 days, respectively); M12 (17, 39 and 190 days, respectively). Pharmacokinetic and pharmacodynamic testing after treatment in orthotopic GBM43 tumors showed inhibitory levels of WSD0628 and a reduction of γH2AX foci in the combination-treated tumors.
Collectively, these results suggest a promising role for WSD0628 in combination with RT in brain tumors and provide the rationale for an ongoing Phase 0/1A clinical trial testing this combination in recurrent GBM.
Accepted manuscriptsAuthor notes
Zhiyi Xue and Ann C. Mladek Equal first author contribution
