| Literature DB >> 31236944 |
Gian Luca Negri1,2, Bruno M Grande3, Alberto Delaidelli1,4, Amal El-Naggar1,5, Dawn Cochrane1, Ching C Lau6, Timothy J Triche7,8, Richard A Moore2, Steven Jm Jones2, Alexandre Montpetit9, Marco A Marra2,10, David Malkin11, Ryan D Morin3, Poul H Sorensen1,4.
Abstract
Despite being the most common childhood bone tumor, the genomic characterization of osteosarcoma remains incomplete. In particular, very few osteosarcoma metastases have been sequenced to date, critical to better understand mechanisms of progression and evolution in this tumor. We performed an integrated whole genome and exome sequencing analysis of paired primary and metastatic pediatric osteosarcoma specimens to identify recurrent genomic alterations. Sequencing of 13 osteosarcoma patients including 13 primary, 10 metastatic, and 3 locally recurring tumors revealed a highly heterogeneous mutational landscape, including cases of hypermutation and microsatellite instability positivity, but with virtually no recurrent alterations except for mutations involving the tumor suppressor genes RB1 and TP53. At the germline level, we detected alterations in multiple cancer related genes in the majority of the cohort, including those potentially disrupting DNA damage response pathways. Metastases retained only a minimal number of short variants from their corresponding primary tumors, while copy number alterations showed higher conservation. One recurrently amplified gene, KDR, was highly expressed in advanced cases and associated with poor prognosis.Entities:
Keywords: KDR; VEGF; childhood bone sarcomas; genome sequencing; metastasis; osteosarcoma
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Year: 2019 PMID: 31236944 PMCID: PMC9263032 DOI: 10.1002/path.5319
Source DB: PubMed Journal: J Pathol ISSN: 0022-3417 Impact factor: 9.883