Chromosome Instability Accounts for Reverse Metastatic Outcomes of Pediatric and Adult Synovial Sarcomas

Author:

Lagarde Pauline1,Przybyl Joanna1,Brulard Céline1,Pérot Gaëlle1,Pierron Gaelle1,Delattre Olivier1,Sciot Raf1,Wozniak Agnieszka1,Schöffski Patrick1,Terrier Philippe1,Neuville Agnès1,Coindre Jean-Michel1,Italiano Antoine1,Orbach Daniel1,Debiec-Rychter Maria1,Chibon Frédéric1

Affiliation:

1. Pauline Lagarde, Céline Brulard, Gaëlle Pérot, Agnès Neuville, Jean-Michel Coindre, and Frédéric Chibon, Institut National de la Santé et de la Recherche Médicale (INSERM) U916-Institut Bergonié; Pauline Lagarde, Gaëlle Pérot, Agnès Neuville, Jean-Michel Coindre, Antoine Italiano, and Frédéric Chibon, Institut Bergonié; Jean-Michel Coindre, Université Victor Segalen Bordeaux 2, Bordeaux; Gaelle Pierron, Olivier Delattre, Daniel Orbach, Institut Curie; Olivier Delattre, INSERM 830, Institut Curie, Paris;...

Abstract

PurposeSynovial sarcoma (SS) occurs in both children and adults, although metastatic events are much more common in adults. Whereas the importance of the t(X;18) translocation in SS oncogenesis is well established, the genetic basis of SS metastasis is still poorly understood. We recently reported expression (CINSARC; Complexity Index in Sarcoma) and Genomic Index prognostic signatures related to chromosome integrity in sarcomas and GI stromal tumors. Here we investigate whether these signatures can also predict outcomes in SS.Patients and MethodsOne hundred patients who had primary untreated SS tumors were selected for expression and genomic profiling in a training/validation approach.ResultsCINSARC and Genomic Index have strong independent and validated prognostic values (P < .001). By comparing expression profiles of tumors with or without metastasis, 14 genes that are common to the CINSARC signature were identified, and the two top-ranked genes, KIF14 and CDCA2, were validated as prognostic markers in an independent cohort. Comparing genomic profiles of adult versus pediatric SS, we show that metastasis is associated with genome complexity in both situations and that the adult genome is more frequently rearranged. Accordingly, pediatric patients with an even genomic profile do not develop metastasis.ConclusionMetastasis development in SS is strongly associated with chromosome complexity, and CINSARC and Genomic Index are validated independent prognostic factors. The differences in metastasis frequency between adults and children are associated with genome instability, which is much more frequent in adults. Genomic Index is potentially the best overall biomarker and clearly the most clinically relevant, considering that genome profiling from formalin-fixed samples is already used in pathology.

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

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