Recurrent rearrangements of FOS and FOSB define osteoblastoma

Matthew W. Fittall; William Mifsud; Nischalan Pillay; Hongtao Ye; Anna‐Christina Strobl; Annelien Verfaillie; Jonas Demeulemeester; Lei Zhang; Fitim Berisha; Maxime Tarabichi; Matthew D. Young; Elena Miranda; Patrick Tarpey; Roberto Tirabosco; Fernanda Amary; Agamemnon E. Grigoriadis; Michael R. Stratton; Peter Van Loo; Cristina R. Antonescu; Peter J. Campbell; Adrienne M. Flanagan; Sam Behjati

doi:10.1038/s41467-018-04530-z

Recurrent rearrangements of FOS and FOSB define osteoblastoma

Matthew W. Fittall(The Francis Crick Institute), William Mifsud(Great Ormond Street Hospital for Children NHS Foundation Trust), Nischalan Pillay(Royal National Orthopaedic Hospital), Hongtao Ye(Royal National Orthopaedic Hospital), Anna‐Christina Strobl(Royal National Orthopaedic Hospital), Annelien Verfaillie(The Francis Crick Institute), Jonas Demeulemeester(The Francis Crick Institute), Lei Zhang(Memorial Sloan Kettering Cancer Center), Fitim Berisha(Royal National Orthopaedic Hospital), Maxime Tarabichi(The Francis Crick Institute), Matthew D. Young(Wellcome Sanger Institute), Elena Miranda(London Cancer), Patrick Tarpey(Wellcome Sanger Institute), Roberto Tirabosco(Royal National Orthopaedic Hospital), Fernanda Amary(Royal National Orthopaedic Hospital), Agamemnon E. Grigoriadis(Guy's Hospital), Michael R. Stratton(Wellcome Sanger Institute), Peter Van Loo(The Francis Crick Institute), Cristina R. Antonescu(Memorial Sloan Kettering Cancer Center), Peter J. Campbell(Wellcome Sanger Institute), Adrienne M. Flanagan(Cancer Research UK), Sam Behjati(University of Cambridge)

Nature Communications

May 25, 2018

10.1038/s41467-018-04530-z

Cited by 149Open Access

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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.

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