Therapeutic Relevance of Molecular Screening Program in Patients with Metastatic Sarcoma: Analysis from the ProfiLER 01 Trial

Overview

Journal Transl Oncol

Specialty Oncology

Date 2020 Sep 20

PMID 32950930

Citations 6

Authors

Patrick Arnaud-Coffin

Mehdi Brahmi

Helene Vanacker

Lauriane Eberst

Olivier Tredan

Valery Attignon

Daniel Pissaloux

Emilie Sohier

Philippe Cassier

Gwenaelle Garin

David Perol

Jean-Yves Blay

Armelle Dufresne

Affiliations

Soon will be listed here.

Abstract

Background: Advanced sarcoma is a group of heterogeneous disease with poor prognosis and poor efficacy of medical treatment. They represent a promising group of tumors to assess molecular-based therapy (MBT) strategy.

Patients And Methods: Genomic profiles of patients with advanced sarcoma included in the ProfiLER program were established by NGS using a 69 genes panel and CGH array. A weekly molecular board reviewed genomic reports to select relevant genomic alterations and propose recommendations for MBT.

Results: A genomic profile was available for 158 of 164 patients. At least 1 relevant genomic alteration was reported for 106 patients (67%), with frequent multiple alterations (68%). In total, 289 relevant genomic alterations were identified in 143 different genes; 139 homozygous deletions, 86 gene amplifications and 64 somatic mutations. The most frequently impacted genes were TP53, Rb1, CDKN2A, CDK4, MDM2, and PTEN. MBT was recommended for 47 patients and initiated for 13 patients. One objective response was observed for an angiosarcoma treated with pazopanib for FLT4 amplification; 4 patients had a stable disease, including a long-lasting 33 months stabilization.

Conclusion: Genomic profiling for advanced sarcoma is feasible, even for bone sarcoma. A small proportion of patients are eventually treated with MBT, similar to other tumor types. We could not demonstrate this strategy to be beneficial to patients. Our data suggest that molecular profiling should not be used in routine practice but warrants further exploration in clinical trials, focusing on sarcoma with complex genomic, and adding transcriptomic analysis to the copy number and mutational analyses.

Citing Articles

The French multicentric molecular analysis platforms and personalized medicine trials MOST, MOST Plus and MEGAMOST.

Verlingue L, Desevre M, Polito M, Garin G, Rodriguez C, Qing W Acta Oncol. 2024; 63:411-417.

PMID: 38807312 PMC: 11332485. DOI: 10.2340/1651-226X.2024.32745.

Genomic Profiling and Clinical Outcomes of Targeted Therapies in Adult Patients with Soft Tissue Sarcomas.

Kokkali S, Georgaki E, Mandrakis G, Valverde C, Theocharis S Cells. 2023; 12(22).

PMID: 37998367 PMC: 10670373. DOI: 10.3390/cells12222632.

Targeted Treatment of Soft-Tissue Sarcoma.

Riskjell A, Makinen V, Sandfeld-Paulsen B, Aggerholm-Pedersen N J Pers Med. 2023; 13(5).

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Case report: Unique FLT4 variants associated with differential response to anlotinib in angiosarcoma.

Gu Y, Meng J, Ju Y, You X, Sun T, Lu J Front Oncol. 2022; 12:1027696.

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The diagnostic utility of DNA copy number analysis of core needle biopsies from soft tissue and bone tumors.

Koster J, Piccinelli P, Arvidsson L, Vult von Steyern F, De Mattos C, Almquist M Lab Invest. 2022; 102(8):838-845.

PMID: 35318454 PMC: 9309094. DOI: 10.1038/s41374-022-00770-2.

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