<i>IDH1</i> and <i>IDH2</i> mutations are frequent events in central chondrosarcoma and central and periosteal chondromas but not in other mesenchymal tumours

Maria Fernanda Amary(Royal National Orthopaedic Hospital), Krisztián Bácsi(Royal National Orthopaedic Hospital NHS Trust), Francesca Maggiani(Royal National Orthopaedic Hospital NHS Trust), Stephen Damato(Royal National Orthopaedic Hospital NHS Trust), Dina Halai(Royal National Orthopaedic Hospital NHS Trust), Fitim Berisha(Royal National Orthopaedic Hospital NHS Trust), Robin Pollock(Royal National Orthopaedic Hospital NHS Trust), Paul O’Donnell(Royal National Orthopaedic Hospital NHS Trust), Anita Grigoriadis(Guy's Hospital), Tim C. Diss(UCL Australia), Malihe Eskandarpour(UCL Australia), Nadège Presneau(UCL Australia), Pancras C.W. Hogendoorn(Leiden University), P. Andrew Futreal(Wellcome Sanger Institute), Roberto Tirabosco(Royal National Orthopaedic Hospital NHS Trust), Adrienne M. Flanagan(Royal National Orthopaedic Hospital NHS Trust)
The Journal of Pathology
April 7, 2011
10.1002/path.2913
Cited by 992Open Access
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Abstract

Somatic mutations in isocitrate dehydrogenase 1 (IDH1) and IDH2 occur in gliomas and acute myeloid leukaemia (AML). Since patients with multiple enchondromas have occasionally been reported to have these conditions, we hypothesized that the same mutations would occur in cartilaginous neoplasms. Approximately 1200 mesenchymal tumours, including 220 cartilaginous tumours, 222 osteosarcomas and another ∼750 bone and soft tissue tumours, were screened for IDH1 R132 mutations, using Sequenom(®) mass spectrometry. Cartilaginous tumours and chondroblastic osteosarcomas, wild-type for IDH1 R132, were analysed for IDH2 (R172, R140) mutations. Validation was performed by capillary sequencing and restriction enzyme digestion. Heterozygous somatic IDH1/IDH2 mutations, which result in the production of a potential oncometabolite, 2-hydroxyglutarate, were only detected in central and periosteal cartilaginous tumours, and were found in at least 56% of these, ∼40% of which were represented by R132C. IDH1 R132H mutations were confirmed by immunoreactivity for this mutant allele. The ratio of IDH1:IDH2 mutation was 10.6 : 1. No IDH2 R140 mutations were detected. Mutations were detected in enchondromas through to conventional central and dedifferentiated chondrosarcomas, in patients with both solitary and multiple neoplasms. No germline mutations were detected. No mutations were detected in peripheral chondrosarcomas and osteochondromas. In conclusion, IDH1 and IDH2 mutations represent the first common genetic abnormalities to be identified in conventional central and periosteal cartilaginous tumours. As in gliomas and AML, the mutations appear to occur early in tumourigenesis. We speculate that a mosaic pattern of IDH-mutation-bearing cells explains the reports of diverse tumours (gliomas, AML, multiple cartilaginous neoplasms, haemangiomas) occurring in the same patient.

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