Feasibility of multiomics tumor profiling for guiding treatment of melanoma

医学 置信区间 肿瘤科 内科学 观察研究
作者
Nicola Miglino,Nora C. Toussaint,Alexander Ring,Ximena Bonilla,Marina Tusup,Benedict Gosztonyi,Tarun Mehra,Gabriele Gut,Francis Jacob,Stéphane Chevrier,Kjong-Van Lehmann,Ruben Casanova,Alice K. Jacobs,Sujana Sivapatham,Laura Amanda Boos,Parisa Rahimzadeh,Manuel Schuerch,Bettina Sobottka,Natalia Chicherova,Shuqing Yu
出处
期刊:Nature Medicine [Nature Portfolio]
标识
DOI:10.1038/s41591-025-03715-6
摘要

Abstract There is limited evidence supporting the feasibility of using omics and functional technologies to inform treatment decisions. Here we present results from a cohort of 116 melanoma patients in the prospective, multicentric observational Tumor Profiler (TuPro) precision oncology project. Nine independent technologies, mostly at single-cell level, were used to analyze 126 patient samples, generating up to 500 Gb of data per sample (40,000 potential markers) within 4 weeks. Among established and experimental markers, the molecular tumor board selected 54 to inform its treatment recommendations. In 75% of cases, TuPro-based data were judged to be useful in informing recommendations. Patients received either standard of care (SOC) treatments or highly individualized, polybiomarker-driven treatments (beyond SOC). The objective response rate in difficult-to-treat palliative, beyond SOC patients ( n = 37) was 38%, with a disease control rate of 54%. Progression-free survival of patients with TuPro-informed therapy decisions was 6.04 months, (95% confidence interval, 3.75–12.06) and 5.35 months (95% confidence interval, 2.89–12.06) in ≥third therapy lines. The proof-of-concept TuPro project demonstrated the feasibility and relevance of omics-based tumor profiling to support data-guided clinical decision-making. ClinicalTrials.gov identifier: NCT06463509 .
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