Genomic analyses of gynaecologic carcinosarcomas reveal frequent mutations in chromatin remodelling genes

Siân Jones; Nicolas Stransky; Christine L. McCord; Ethan Cerami; James Lagowski; Devon Kelly; Samuel V. Angiuoli; Mark Sausen; Lisa Kann; Manish Shukla; Rosemary Makar; Laura D. Wood; Luis A. Diaz; Christoph Lengauer; Victor E. Velculescu

doi:10.1038/ncomms6006

Genomic analyses of gynaecologic carcinosarcomas reveal frequent mutations in chromatin remodelling genes

Siân Jones, Nicolas Stransky, Christine L. McCord, Ethan Cerami, James Lagowski, Devon Kelly, Samuel V. Angiuoli, Mark Sausen, Lisa Kann, Manish Shukla, Rosemary Makar, Laura D. Wood, Luis A. Diaz, Christoph Lengauer, Victor E. Velculescu

School of Medicine

Research output: Contribution to journal › Article › peer-review

98 Scopus citations

Abstract

Malignant mixed Müllerian tumours, also known as carcinosarcomas, are rare tumours of gynaecological origin. Here we perform whole-exome analyses of 22 tumours using massively parallel sequencing to determine the mutational landscape of this tumour type. On average, we identify 43 mutations per tumour, excluding four cases with a mutator phenotype that harboured inactivating mutations in mismatch repair genes. In addition to mutations in TP53 and KRAS, we identify genetic alterations in chromatin remodelling genes, ARID1A and ARID1B, in histone methyltransferase MLL3, in histone deacetylase modifier SPOP and in chromatin assembly factor BAZ1A, in nearly two thirds of cases. Alterations in genes with potential clinical utility are observed in more than three quarters of the cases and included members of the PI3-kinase and homologous DNA repair pathways. These findings highlight the importance of the dysregulation of chromatin remodelling in carcinosarcoma tumorigenesis and suggest new avenues for personalized therapy.

Original language	English (US)
Article number	5006
Journal	Nature communications
Volume	5
DOIs	https://doi.org/10.1038/ncomms6006
State	Published - 2014

ASJC Scopus subject areas

General Chemistry
General Biochemistry, Genetics and Molecular Biology
General Physics and Astronomy

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Jones, S., Stransky, N., McCord, C. L., Cerami, E., Lagowski, J., Kelly, D., Angiuoli, S. V., Sausen, M., Kann, L., Shukla, M., Makar, R., Wood, L. D., Diaz, L. A., Lengauer, C., & Velculescu, V. E. (2014). Genomic analyses of gynaecologic carcinosarcomas reveal frequent mutations in chromatin remodelling genes. Nature communications, 5, Article 5006. https://doi.org/10.1038/ncomms6006

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title = "Genomic analyses of gynaecologic carcinosarcomas reveal frequent mutations in chromatin remodelling genes",

abstract = "Malignant mixed M{\"u}llerian tumours, also known as carcinosarcomas, are rare tumours of gynaecological origin. Here we perform whole-exome analyses of 22 tumours using massively parallel sequencing to determine the mutational landscape of this tumour type. On average, we identify 43 mutations per tumour, excluding four cases with a mutator phenotype that harboured inactivating mutations in mismatch repair genes. In addition to mutations in TP53 and KRAS, we identify genetic alterations in chromatin remodelling genes, ARID1A and ARID1B, in histone methyltransferase MLL3, in histone deacetylase modifier SPOP and in chromatin assembly factor BAZ1A, in nearly two thirds of cases. Alterations in genes with potential clinical utility are observed in more than three quarters of the cases and included members of the PI3-kinase and homologous DNA repair pathways. These findings highlight the importance of the dysregulation of chromatin remodelling in carcinosarcoma tumorigenesis and suggest new avenues for personalized therapy.",

author = "Si{\^a}n Jones and Nicolas Stransky and McCord, {Christine L.} and Ethan Cerami and James Lagowski and Devon Kelly and Angiuoli, {Samuel V.} and Mark Sausen and Lisa Kann and Manish Shukla and Rosemary Makar and Wood, {Laura D.} and Diaz, {Luis A.} and Christoph Lengauer and Velculescu, {Victor E.}",

year = "2014",

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AU - Jones, Siân

AU - Stransky, Nicolas

AU - McCord, Christine L.

AU - Cerami, Ethan

AU - Lagowski, James

AU - Kelly, Devon

AU - Angiuoli, Samuel V.

AU - Sausen, Mark

AU - Kann, Lisa

AU - Shukla, Manish

AU - Makar, Rosemary

AU - Wood, Laura D.

AU - Diaz, Luis A.

AU - Lengauer, Christoph

AU - Velculescu, Victor E.

PY - 2014

Y1 - 2014

N2 - Malignant mixed Müllerian tumours, also known as carcinosarcomas, are rare tumours of gynaecological origin. Here we perform whole-exome analyses of 22 tumours using massively parallel sequencing to determine the mutational landscape of this tumour type. On average, we identify 43 mutations per tumour, excluding four cases with a mutator phenotype that harboured inactivating mutations in mismatch repair genes. In addition to mutations in TP53 and KRAS, we identify genetic alterations in chromatin remodelling genes, ARID1A and ARID1B, in histone methyltransferase MLL3, in histone deacetylase modifier SPOP and in chromatin assembly factor BAZ1A, in nearly two thirds of cases. Alterations in genes with potential clinical utility are observed in more than three quarters of the cases and included members of the PI3-kinase and homologous DNA repair pathways. These findings highlight the importance of the dysregulation of chromatin remodelling in carcinosarcoma tumorigenesis and suggest new avenues for personalized therapy.

AB - Malignant mixed Müllerian tumours, also known as carcinosarcomas, are rare tumours of gynaecological origin. Here we perform whole-exome analyses of 22 tumours using massively parallel sequencing to determine the mutational landscape of this tumour type. On average, we identify 43 mutations per tumour, excluding four cases with a mutator phenotype that harboured inactivating mutations in mismatch repair genes. In addition to mutations in TP53 and KRAS, we identify genetic alterations in chromatin remodelling genes, ARID1A and ARID1B, in histone methyltransferase MLL3, in histone deacetylase modifier SPOP and in chromatin assembly factor BAZ1A, in nearly two thirds of cases. Alterations in genes with potential clinical utility are observed in more than three quarters of the cases and included members of the PI3-kinase and homologous DNA repair pathways. These findings highlight the importance of the dysregulation of chromatin remodelling in carcinosarcoma tumorigenesis and suggest new avenues for personalized therapy.

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Genomic analyses of gynaecologic carcinosarcomas reveal frequent mutations in chromatin remodelling genes

Abstract

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