Clinical Impact of Prospective Whole Genome Sequencing in Sarcoma Patients

Author:

Schipper Luuk J.,Monkhorst Kim,Samsom Kris G.,Bosch Linda J.W.,Snaebjornsson Petur,van Boven Hester,Roepman Paul,van der Kolk Lizet E.,van Houdt Winan J.ORCID,van der Graaf Winette T.A.ORCID,Meijer Gerrit A.,Voest Emile E.ORCID

Abstract

With more than 70 different histological sarcoma subtypes, accurate classification can be challenging. Although characteristic genetic events can largely facilitate pathological assessment, large-scale molecular profiling generally is not part of regular diagnostic workflows for sarcoma patients. We hypothesized that whole genome sequencing (WGS) optimizes clinical care of sarcoma patients by detection of diagnostic and actionable genomic characteristics, and of underlying hereditary conditions. WGS of tumor and germline DNA was incorporated in the diagnostic work-up of 83 patients with a (presumed) sarcomas in a tertiary referral center. Clinical follow-up data were collected prospectively to assess impact of WGS on clinical decision making. In 12/83 patients (14%), the genomic profile led to revision of cancer diagnosis, with change of treatment plan in eight. All twelve patients had undergone multiple tissue retrieval procedures and immunohistopathological assessments by regional and expert pathologists prior to WGS analysis. Actionable biomarkers with therapeutic potential were identified for 30/83 patients. Pathogenic germline variants were present in seven patients. In conclusion, unbiased genomic characterization with WGS identifies genomic biomarkers with direct clinical implications for sarcoma patients. Given the diagnostic complexity and high unmet need for new treatment opportunities in sarcoma patients, WGS can be an important extension of the diagnostic arsenal of pathologists.

Funder

Netherlands Organisation for Health Research and Development

Hartwig Medical Foundation

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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