Non-chemotherapy Adjuvant Agents in TP53 Mutant Ewing Sarcoma

Overview

Journal Sci Rep

Specialty Science

Date 2023 Sep 1

PMID 37658148

Authors

Jin-Ah Kim

Kenneth A Crawford

Piero A Spada

Leah R Martin

Jiaqi Zhang

Rain Wong

Joel M Reid

Clinton F Stewart

Timothy M Frank

Qianqian Liu

Joel E Michalek

Charles Keller

Affiliations

Soon will be listed here.

Abstract

Ewing sarcoma (EWS) is a malignant tumor arising in bone or soft tissue that occurs in adolescent and young adult patients as well as adults later in life. Although non-metastatic EWS is typically responsive to treatment when newly diagnosed, relapsed cases have an unmet need for which no standard treatment approach exists. Recent phase III clinical trials for EWS comparing 7 vs 5 chemotherapy drugs have failed to improve survival. To extend the durability of remission for EWS, we investigated 3 non-chemotherapy adjuvant therapy drug candidates to be combined with chemotherapy. The efficacy of these adjuvant drugs was investigated via anchorage-dependent growth assays, anchorage-independent soft-agar colony formation assays and EWS xenograft mouse models. Enoxacin and entinostat were the most effective adjuvant drug in both long-term in vitro and in vivo adjuvant studies. In the context that enoxacin is an FDA-approved antibiotic, and that entinostat is an investigational agent not yet FDA-approved, we propose enoxacin as an adjuvant drug for further preclinical and clinical investigation in EWS patients.

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