Literature DB >> 26248895

GNAS mutations are not detected in parosteal and low-grade central osteosarcomas.

Carolina Salinas-Souza1,2, Carlos De Andrea1,3, Michel Bihl4, Michal Kovac5, Nischalan Pillay3,6, Tim Forshew6, Alice Gutteridge6, Hongtao Ye3, M Fernanda Amary3,6, Roberto Tirabosco3, Silvia Regina Caminada Toledo2, Daniel Baumhoer5, Adrienne M Flanagan3,6.   

Abstract

Parosteal osteosarcoma, low-grade central osteosarcoma, and fibrous dysplasia share similar histological features that may pose a diagnostic challenge. The detection of GNAS mutations in primary bone tumors has been useful in clinical practice for diagnosing fibrous dysplasia. However, the recent report of GNAS mutations being detected in a significant proportion of parosteal osteosarcoma challenges the specificity of this mutation. As the number of cases reported in this study was small we set out to determine if these results could be reproduced. We studied 97 formalin-fixed paraffin-embedded low-grade osteosarcomas from 90 patients including 62 parosteal osteosarcomas, of which MDM2 amplification was detected in 79%, 11 periosteal osteosarcomas and 24 low-grade central osteosarcoma samples. The mutational status of GNAS was analyzed in codons p.R201, p.Q227, and other less common GNAS alterations by bidirectional Sanger sequencing and/or next generation sequencing using the Life Technologies Ion Torrent platform. GNAS mutations were not detected in any of the low-grade osteosarcomas from which informative DNA was extracted. Our findings therefore support prior observations that GNAS mutations are highly specific for fibrous dysplasia and occur rarely, if ever, in parosteal and other low-grade osteosarcomas.

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Year:  2015        PMID: 26248895     DOI: 10.1038/modpathol.2015.91

Source DB:  PubMed          Journal:  Mod Pathol        ISSN: 0893-3952            Impact factor:   7.842


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Journal:  Pathologe       Date:  2018-03       Impact factor: 1.011

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Review 10.  Systematic target actionability reviews of preclinical proof-of-concept papers to match targeted drugs to paediatric cancers.

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Journal:  Eur J Cancer       Date:  2020-03-27       Impact factor: 9.162

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