Approaches to identifying drug resistance mechanisms to clinically relevant treatments in childhood rhabdomyosarcoma

Samson Ghilu; Christopher L Morton; Angelina V Vaseva; Siyuan Zheng; Raushan T Kurmasheva; Peter J Houghton

doi:10.20517/cdr.2021.112

Approaches to identifying drug resistance mechanisms to clinically relevant treatments in childhood rhabdomyosarcoma

Cancer Drug Resist. 2022;5(1):80-89. doi: 10.20517/cdr.2021.112. Epub 2022 Jan 4.

Authors

Samson Ghilu¹, Christopher L Morton², Angelina V Vaseva¹, Siyuan Zheng³, Raushan T Kurmasheva¹, Peter J Houghton¹

Affiliations

¹ Department of Molecular Medicine, Greehey Children's Cancer Research Institute, UT Health, San Antonio, TX 78229, USA.
² Department of Surgery, St. Jude Children's Research Hospital, Memphis, TN 38105, USA.
³ Department of Epidemiology and Biostatistics, Greehey Children's Cancer Research Institute, UT Health, San Antonio, TX 78229, USA.

Abstract

Aim: Despite aggressive multiagent protocols, patients with metastatic rhabdomyosarcoma (RMS) have poor prognosis. In a recent high-risk trial (ARST0431), 25% of patients failed within the first year, while on therapy and 80% had tumor progression within 24 months. However, the mechanisms for tumor resistance are essentially unknown. Here we explore the use of preclinical models to develop resistance to complex chemotherapy regimens used in ARST0431.

Methods: A Single Mouse Testing (SMT) protocol was used to evaluate the sensitivity of 34 RMS xenograft models to one cycle of vincristine, actinomycin D, cyclophosphamide (VAC) treatment. Tumor response was determined by caliper measurement, and tumor regression and event-free survival (EFS) were used as endpoints for evaluation. Treated tumors at regrowth were transplanted into recipient mice, and the treatment was repeated until tumors progressed during the treatment period (i.e., became resistant). At transplant, tumor tissue was stored for biochemical and omics analysis.

Results: The sensitivity to VAC of 34 RMS models was determined. EFS varied from 3 weeks to > 20 weeks. Tumor models were classified as having intrinsic resistance, intermediate sensitivity, or high sensitivity to VAC therapy. Resistance to VAC was developed in multiple models after 2-5 cycles of therapy; however, there were examples where sensitivity remained unchanged after 3 cycles of treatment.

Conclusion: The SMT approach allows for in vivo assessment of drug sensitivity and development of drug resistance in a large number of RMS models. As such, it provides a platform for assessing in vivo drug resistance mechanisms at a "population" level, simulating conditions in vivo that lead to clinical resistance. These VAC-resistant models represent "high-risk" tumors that mimic a preclinical phase 2 population and will be valuable for identifying novel agents active against VAC-resistant disease.

Keywords: Rhabdomyosarcoma; acquired drug resistance; combination therapy; intrinsic drug resistance; patient-derived xenografts.

Abstract

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