A genetic model for central chondrosarcoma evolution correlates with patient outcome.

Cross, William; Lyskjær, Iben; Lesluyes, Tom; Hargreaves, Steven; Strobl, Anna-Christina; Davies, Christopher; Waise, Sara; Hames-Fathi, Shadi; Oukrif, Dahmane; Ye, Hongtao; Amary, Fernanda; Tirabosco, Roberto; Gerrand, Craig; Baker, Toby; Barnes, David; Steele, Christopher; Alexandrov, Ludmil; Bond, Gareth; Cool, Paul; Pillay, Nischalan; Van Loo, Peter; Flanagan, Adrienne M

Cross, William; Lyskjær, Iben; Lesluyes, Tom; Hargreaves, Steven; Strobl, Anna-Christina; Davies, Christopher; Waise, Sara; Hames-Fathi, Shadi; Oukrif, Dahmane; Ye, Hongtao; Amary, Fernanda; Tirabosco, Roberto; Gerrand, Craig; Baker, Toby; Barnes, David; Steele, Christopher; Alexandrov, Ludmil; Bond, Gareth; Cool, Paul; Pillay, Nischalan; Van Loo, Peter; Flanagan, Adrienne M.

Afiliação

Cross W; Research Department of Pathology, University College London, UCL Cancer Institute, London, UK.
Lyskjær I; Research Department of Pathology, University College London, UCL Cancer Institute, London, UK.
Lesluyes T; Medical Genomics Research Group, University College London, UCL Cancer Institute, London, UK.
Hargreaves S; The Francis Crick Institute, London, UK.
Strobl AC; Research Department of Pathology, University College London, UCL Cancer Institute, London, UK.
Davies C; Department of Histopathology, Royal National Orthopaedic Hospital, Stanmore, UK.
Waise S; Research Department of Pathology, University College London, UCL Cancer Institute, London, UK.
Hames-Fathi S; Department of Histopathology, Royal National Orthopaedic Hospital, Stanmore, UK.
Oukrif D; The Francis Crick Institute, London, UK.
Ye H; Cancer Sciences Unit, University of Southampton, Southampton, UK.
Amary F; Research Department of Pathology, University College London, UCL Cancer Institute, London, UK.
Tirabosco R; Research Department of Pathology, University College London, UCL Cancer Institute, London, UK.
Gerrand C; Department of Histopathology, Royal National Orthopaedic Hospital, Stanmore, UK.
Baker T; Department of Histopathology, Royal National Orthopaedic Hospital, Stanmore, UK.
Barnes D; Department of Histopathology, Royal National Orthopaedic Hospital, Stanmore, UK.
Steele C; Bone Tumour Unit, Royal National Orthopaedic Hospital, Stanmore, UK.
Alexandrov L; The Francis Crick Institute, London, UK.
Bond G; Institute of Cancer and Genomic Sciences, Birmingham University, Birmingham, UK.
Cool P; University of California, San Diego, USA.
Pillay N; Institute of Cancer and Genomic Sciences, Birmingham University, Birmingham, UK.
Flanagan AM; Robert Jones & Agnes Hunt Orthopaedic Hospital NHS Foundation Trust, Oswestry, UK.

Genome Med ; 14(1): 99, 2022 08 30.

Article em En | MEDLINE | ID: mdl-36042521

ABSTRACT

ABSTRACT

BACKGROUND:

Central conventional chondrosarcoma (CS) is the most common subtype of primary malignant bone tumour in adults. Treatment options are usually limited to surgery, and prognosis is challenging. These tumours are characterised by the presence and absence of IDH1 and IDH2 mutations, and recently, TERT promoter alterations have been reported in around 20% of cases. The effect of these mutations on clinical outcome remains unclear. The purpose of this study was to determine if prognostic accuracy can be improved by the addition of genomic data, and specifically by examination of IDH1, IDH2, and TERT mutations.

METHODS:

In this study, we combined both archival samples and data sourced from the Genomics England 100,000 Genomes Project (n = 356). Mutations in IDH1, IDH2, and TERT were profiled using digital droplet PCR (n = 346), whole genome sequencing (n=68), or both (n = 64). Complex events and other genetic features were also examined, along with methylation array data (n = 84). We correlated clinical features and patient outcomes with our genetic findings.

RESULTS:

IDH2-mutant tumours occur in older patients and commonly present with high-grade or dedifferentiated disease. Notably, TERT mutations occur most frequently in IDH2-mutant tumours, although have no effect on survival in this group. In contrast, TERT mutations are rarer in IDH1-mutant tumours, yet they are associated with a less favourable outcome in this group. We also found that methylation profiles distinguish IDH1- from IDH2-mutant tumours. IDH wild-type tumours rarely exhibit TERT mutations and tend to be diagnosed in a younger population than those with tumours harbouring IDH1 and IDH2 mutations. A major genetic feature of this group is haploidisation and subsequent genome doubling. These tumours evolve less frequently to dedifferentiated disease and therefore constitute a lower risk group.

CONCLUSIONS:

Tumours with IDH1 or IDH2 mutations or those that are IDHwt have significantly different genetic pathways and outcomes in relation to TERT mutation. Diagnostic testing for IDH1, IDH2, and TERT mutations could therefore help to guide clinical monitoring and prognostication.

Assuntos

Neoplasias Ósseas; Condrossarcoma; Adulto; Idoso; Neoplasias Ósseas/genética; Neoplasias Ósseas/patologia; Condrossarcoma/genética; Condrossarcoma/patologia; Humanos; Isocitrato Desidrogenase/genética; Modelos Genéticos; Mutação; Prognóstico

Palavras-chave

Cancer evolution; Chondrosarcoma; Genetics; Genomics; IDH1; IDH2; Sarcoma; TERT

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Neoplasias Ósseas / Condrossarcoma Idioma: En Ano de publicação: 2022 Tipo de documento: Article

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PubMed Links

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Neoplasias Ósseas / Condrossarcoma Idioma: En Ano de publicação: 2022 Tipo de documento: Article