Start Over

Recurrent rearrangements of FOS and FOSB define osteoblastoma

Authors :: Nischalan Pillay
Michael R. Stratton
Lei Zhang
William Mifsud
Matthew Fittall
Roberto Tirabosco
Patrick S. Tarpey
Hongtao Ye
Elena Miranda
Sam Behjati
Jonas Demeulemeester
Cristina R. Antonescu
Fernanda Amary
Peter Van Loo
Annelien Verfaillie
Peter J. Campbell
Anna Christina Strobl
Agamemnon E. Grigoriadis
Maxime Tarabichi
Fitim Berisha
Matthew D. Young
Adrienne M. Flanagan
Fittall, Matthew W [0000-0002-5172-4100]
Pillay, Nischalan [0000-0003-0579-4105]
Demeulemeester, Jonas [0000-0002-2660-2478]
Van Loo, Peter [0000-0003-0292-1949]
Apollo - University of Cambridge Repository
Source :: Nature Communications, Nature Communications, Vol 9, Iss 1, Pp 1-6 (2018)
Publication Year :: 2018
Publisher :: Nature Publishing Group UK, 2018.
Abstract: The transcription factor FOS has long been implicated in the pathogenesis of bone tumours, following the discovery that the viral homologue, v-fos, caused osteosarcoma in laboratory mice. However, mutations of FOS have not been found in human bone-forming tumours. Here, we report recurrent rearrangement of FOS and its paralogue, FOSB, in the most common benign tumours of bone, osteoblastoma and osteoid osteoma. Combining whole-genome DNA and RNA sequences, we find rearrangement of FOS in five tumours and of FOSB in one tumour. Extending our findings into a cohort of 55 cases, using FISH and immunohistochemistry, provide evidence of ubiquitous mutation of FOS or FOSB in osteoblastoma and osteoid osteoma. Overall, our findings reveal a human bone tumour defined by mutations of FOS and FOSB.<br />FOS has been linked to bone tumour pathogenesis, and viral homologue v-fos causes osteosarcoma in mice. Here, the authors report rearrangement of FOS and its paralogue FOSB in osteoblastoma and osteoid osteoma, revealing human bone tumours that are defined by mutations of FOS and FOSB.