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2 research outputs found

Pan-cancer analysis of homozygous deletions in primary tumours uncovers rare tumour suppressors

Author: Bignell G.R.
Børresen-Dale A.-L.
Campbell P.J.
Cheng J.
Demeulemeester J.
Kristensen V.N.
Lingjærde O.C.
Moreau Y.
Nilsen G.
Nord S.
Pandey B.P.
Pitt J.J.
Russnes H.G.
Stratton M.R.
Van Loo P.
Vollan H.K.M.
Wedge D.C.
White K.P.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2017
Field of study

Homozygous deletions are rare in cancers and often target tumour suppressor genes. Here, we build a compendium of 2218 primary tumours across 12 human cancer types and systematically screen for homozygous deletions, aiming to identify rare tumour suppressors. Our analysis defines 96 genomic regions recurrently targeted by homozygous deletions. These recurrent homozygous deletions occur either over tumour suppressors or over fragile sites, regions of increased genomic instability. We construct a statistical model that separates fragile sites from regions showing signatures of positive selection for homozygous deletions and identify candidate tumour suppressors within those regions. We find 16 established tumour suppressors and propose 27 candidate tumour suppressors. Several of these genes (including MGMT, RAD17, and USP44) show prior evidence of a tumour suppressive function. Other candidate tumour suppressors, such as MAFTRR, KIAA1551, and IGF2BP2, are novel. Our study demonstrates how rare tumour suppressors can be identified through copy number meta-analysis

Oxford University Research Archive

The University of Manchester - Institutional Repository

Recurrent PTPRB and PLCG1 mutations in angiosarcoma

Author: Al Sannaa G.A.
Amary M.F.
Baumhoer D.
Behjati S.
Boshoff C.
Bunney T.D.
Butler A.
Campbell P.J.
Cao Y.
Cooke S.L.
Flanagan A.M.
Futreal P.A.
Gumbs C.
Gundem G.
Halai D.
Hardy C.
Harris A.
Ingram D.
Joseph O.R.
Katan M.
Khatri B.
Koss H.
Lazar A.J.
Little L.
Mahadeshwar H.
Martin S.
Martincorena I.
McDermott U.
Mudie L.
Papaemmanuil E.
Patil M.
Pillay N.
Protopopov A.
Ramakrishna M.
Ravi V.
Roxanis I.
Seth S.
Sheldon H.
Song X.
Steers G.
Stratton M.R.
Tang J.
Tarpey P.S.
Teague J.W.
Tirabosco R.
Torres K.E.
Van Loo P.
Vollan H.K.M.
Wedge D.C.
Zhang J.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 16/03/2014
Field of study

Angiosarcoma is an aggressive malignancy that arises spontaneously or secondarily to ionising radiation or chronic lymphoedema(1). Previous work has identified aberrant angiogenesis, including occasional somatic mutations in angiogenesis signalling genes, as a key driver of angiosarcoma(1). Here, we employed whole genome, exome, and targeted sequencing to study the somatic changes underpinning primary and secondary angiosarcoma. We identified recurrent mutations in two genes, PTPRB and PLCG1, which are intimately linked to angiogenesis. The endothelial phosphatase PTPRB, a negative regulator of vascular growth factor tyrosine kinases, harboured predominantly truncating mutations in 10/39 (26%) tumours. PLCG1, a signal transducer of tyrosine kinases, presented with a recurrent, likely activating R707Q missense variant in 3/34 cases (9%). Overall, 15/39 (38%) tumours harboured at least one driver mutation in angiogenesis signalling genes. Our findings inform and reinforce current therapeutic efforts to target angiogenesis signalling in angiosarcoma

PubMed Central

The University of Manchester - Institutional Repository