What question did this study set out to answer?

This research aims to explore the therapeutic vulnerabilities of sarcomas with homologous recombination deficiencies and identify predictive biomarkers for treatment response.

March 12, 2026Open Access

193P Sensitivity of homologous recombination deficient sarcoma to DNA damage response targeting drugs

Key Points

This research aims to explore the therapeutic vulnerabilities of sarcomas with homologous recombination deficiencies and identify predictive biomarkers for treatment response.
Combined molecular profiling and pharmacotyping of patient-derived sarcoma cells.
Validated gene expression signatures as biomarkers of drug response.
Conducted mid-throughput drug screening on ex vivo sarcoma models.
Analyzed the correlation between SARC-HRD and CINSARC transcriptomic signatures.
Identified a high correlation between SARC-HRD and poor clinical outcomes in sarcoma.
Discovered small inhibitors targeting ATR, CHK1, and WEE1 as potential treatments.
Demonstrated a slowdown of DNA replication forks in treated sarcoma cell models.
Showed increased activation of ATR pathways in sarcoma cells sensitive to DDR inhibitors.

Abstract

Background: Defects in the homologous recombination repair (HRR) pathway have been frequently observed in high-grade ovarian, breast, pancreatic and prostate carcinomas.HRR deficiency (HRD) has emerged as a key therapeutic vulnerability by exploiting the concept of synthetic lethality.Targeting PARP proteins causes cells to rely on other pathways for repairing double-strand DNA breaks.When cells lack functional BRCA1/2 genes or exhibit a compromised HRR pathway, they become sensitive to PARP inhibition (PARPi), while cells with an intact HRR pathway are unaffected.This treatment option is yet to be employed across a broader range of malignancies with HRD traits, like distinct sarcoma subtypes, colorectal carcinoma and hepatocellular carcinoma. Methods:We combined molecular profiling of patients with pharmacotyping of patient-derived sarcoma cells and validated a gene expression signature as predictive biomarker of drug response.Results: Here, we investigated the predictive and prognostic biomarker value of transcriptomic signatures in sarcoma as well as discovered novel therapeutic opportunities within the DDR for soft tissue sarcoma.Firstly, we validated SARC-HRD differential expression in soft tissue sarcoma with HRD traits using an independent cohort.We found a high correlation between SARC-HRD and CINSARC transcriptomic signatures in sarcoma, both associated with poor clinical outcome.Secondly, we performed mid-throughput drug screening in ex vivo patient-derived sarcoma cell models, expressing high levels of both transcriptomic signatures, and identified small inhibitors targeting ATR, CHK1 and WEE1, as single agents or in combination, as promising new treatment strategies for sarcoma patients.Lastly, we showed mechanistically a slowdown of the DNA replication fork upon treatment with selected DDR inhibitors as well as increased ATR pathway activation in sarcoma cell models sensitive to these drugs. Conclusions:In summary, we showed the value of transcriptomic signatures in predicting drug response and offer potential new venues for clinical management of tumors with HRD.

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193P Sensitivity of homologous recombination deficient sarcoma to DNA damage response targeting drugs

Key Points

Abstract

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