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Systematic sequencing of renal carcinoma reveals inactivation of histone modifying genes

Clear cell renal cell carcinoma (ccRCC) is the most common form of adult kidney cancer, characterised by the presence of inactivating mutations in the VHL gene in the majority of cases1,2 and by infrequent somatic mutations in known cancer genes. To elucidate further the genetics of ccRCC, we have s...

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Autores principales: Dalgliesh, Gillian L., Furge, Kyle, Greenman, Chris, Chen, Lina, Bignell, Graham, Butler, Adam, Davies, Helen, Edkins, Sarah, Hardy, Claire, Latimer, Calli, Teague, Jon, Andrews, Jenny, Barthorpe, Syd, Beare, Dave, Buck, Gemma, Campbell, Peter J., Forbes, Simon, Jia, Mingming, Jones, David, Knott, Henry, Kok, Chai Yin, Lau, King Wai, Leroy, Catherine, Lin, Meng-Lay, McBride, David J, Maddison, Mark, Maguire, Simon, McLay, Kirsten, Menzies, Andrew, Mironenko, Tatiana, Mulderrig, Lee, Mudie, Laura, O’Meara, Sarah, Pleasance, Erin, Rajasingham, Arjunan, Shepherd, Rebecca, Smith, Raffaella, Stebbings, Lucy, Stephens, Philip, Tang, Gurpreet, Tarpey, Patrick S, Turrell, Kelly, Dykema, Karl J., Khoo, Sok Kean, Petillo, David, Wondergem, Bill, Anema, John, Kahnoski, Richard J., Teh, Bin Tean, Stratton, Michael R., Futreal, P. Andrew
Formato: Texto
Lenguaje:English
Publicado: 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2820242/
https://www.ncbi.nlm.nih.gov/pubmed/20054297
http://dx.doi.org/10.1038/nature08672
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author Dalgliesh, Gillian L.
Furge, Kyle
Greenman, Chris
Chen, Lina
Bignell, Graham
Butler, Adam
Davies, Helen
Edkins, Sarah
Hardy, Claire
Latimer, Calli
Teague, Jon
Andrews, Jenny
Barthorpe, Syd
Beare, Dave
Buck, Gemma
Campbell, Peter J.
Forbes, Simon
Jia, Mingming
Jones, David
Knott, Henry
Kok, Chai Yin
Lau, King Wai
Leroy, Catherine
Lin, Meng-Lay
McBride, David J
Maddison, Mark
Maguire, Simon
McLay, Kirsten
Menzies, Andrew
Mironenko, Tatiana
Mulderrig, Lee
Mudie, Laura
O’Meara, Sarah
Pleasance, Erin
Rajasingham, Arjunan
Shepherd, Rebecca
Smith, Raffaella
Stebbings, Lucy
Stephens, Philip
Tang, Gurpreet
Tarpey, Patrick S
Turrell, Kelly
Dykema, Karl J.
Khoo, Sok Kean
Petillo, David
Wondergem, Bill
Anema, John
Kahnoski, Richard J.
Teh, Bin Tean
Stratton, Michael R.
Futreal, P. Andrew
author_facet Dalgliesh, Gillian L.
Furge, Kyle
Greenman, Chris
Chen, Lina
Bignell, Graham
Butler, Adam
Davies, Helen
Edkins, Sarah
Hardy, Claire
Latimer, Calli
Teague, Jon
Andrews, Jenny
Barthorpe, Syd
Beare, Dave
Buck, Gemma
Campbell, Peter J.
Forbes, Simon
Jia, Mingming
Jones, David
Knott, Henry
Kok, Chai Yin
Lau, King Wai
Leroy, Catherine
Lin, Meng-Lay
McBride, David J
Maddison, Mark
Maguire, Simon
McLay, Kirsten
Menzies, Andrew
Mironenko, Tatiana
Mulderrig, Lee
Mudie, Laura
O’Meara, Sarah
Pleasance, Erin
Rajasingham, Arjunan
Shepherd, Rebecca
Smith, Raffaella
Stebbings, Lucy
Stephens, Philip
Tang, Gurpreet
Tarpey, Patrick S
Turrell, Kelly
Dykema, Karl J.
Khoo, Sok Kean
Petillo, David
Wondergem, Bill
Anema, John
Kahnoski, Richard J.
Teh, Bin Tean
Stratton, Michael R.
Futreal, P. Andrew
author_sort Dalgliesh, Gillian L.
collection PubMed
description Clear cell renal cell carcinoma (ccRCC) is the most common form of adult kidney cancer, characterised by the presence of inactivating mutations in the VHL gene in the majority of cases1,2 and by infrequent somatic mutations in known cancer genes. To elucidate further the genetics of ccRCC, we have sequenced 101 cases through 3544 protein coding genes. Here we report the identification of inactivating mutations in two genes encoding enzymes involved in histone modification, SETD2, a histone H3 lysine 36 methyltransferase and JARID1C (KDM5C), a histone H3 lysine 4 demethylase in addition to mutations in the histone H3 lysine 27 demethylase, UTX (KMD6A), we recently reported3. The results highlight the role of mutations in components of the chromatin modification machinery in human cancer. Additionally, NF2 mutations were found in non-VHL mutated ccRCC and several other likely cancer genes were identified. These results indicate that substantial genetic heterogeneity exists in a cancer type dominated by mutations in a single gene and that systematic screens will be key to fully elucidating the somatic genetic architecture of cancer.
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spelling pubmed-28202422010-07-21 Systematic sequencing of renal carcinoma reveals inactivation of histone modifying genes Dalgliesh, Gillian L. Furge, Kyle Greenman, Chris Chen, Lina Bignell, Graham Butler, Adam Davies, Helen Edkins, Sarah Hardy, Claire Latimer, Calli Teague, Jon Andrews, Jenny Barthorpe, Syd Beare, Dave Buck, Gemma Campbell, Peter J. Forbes, Simon Jia, Mingming Jones, David Knott, Henry Kok, Chai Yin Lau, King Wai Leroy, Catherine Lin, Meng-Lay McBride, David J Maddison, Mark Maguire, Simon McLay, Kirsten Menzies, Andrew Mironenko, Tatiana Mulderrig, Lee Mudie, Laura O’Meara, Sarah Pleasance, Erin Rajasingham, Arjunan Shepherd, Rebecca Smith, Raffaella Stebbings, Lucy Stephens, Philip Tang, Gurpreet Tarpey, Patrick S Turrell, Kelly Dykema, Karl J. Khoo, Sok Kean Petillo, David Wondergem, Bill Anema, John Kahnoski, Richard J. Teh, Bin Tean Stratton, Michael R. Futreal, P. Andrew Nature Article Clear cell renal cell carcinoma (ccRCC) is the most common form of adult kidney cancer, characterised by the presence of inactivating mutations in the VHL gene in the majority of cases1,2 and by infrequent somatic mutations in known cancer genes. To elucidate further the genetics of ccRCC, we have sequenced 101 cases through 3544 protein coding genes. Here we report the identification of inactivating mutations in two genes encoding enzymes involved in histone modification, SETD2, a histone H3 lysine 36 methyltransferase and JARID1C (KDM5C), a histone H3 lysine 4 demethylase in addition to mutations in the histone H3 lysine 27 demethylase, UTX (KMD6A), we recently reported3. The results highlight the role of mutations in components of the chromatin modification machinery in human cancer. Additionally, NF2 mutations were found in non-VHL mutated ccRCC and several other likely cancer genes were identified. These results indicate that substantial genetic heterogeneity exists in a cancer type dominated by mutations in a single gene and that systematic screens will be key to fully elucidating the somatic genetic architecture of cancer. 2010-01-06 2010-01-21 /pmc/articles/PMC2820242/ /pubmed/20054297 http://dx.doi.org/10.1038/nature08672 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Dalgliesh, Gillian L.
Furge, Kyle
Greenman, Chris
Chen, Lina
Bignell, Graham
Butler, Adam
Davies, Helen
Edkins, Sarah
Hardy, Claire
Latimer, Calli
Teague, Jon
Andrews, Jenny
Barthorpe, Syd
Beare, Dave
Buck, Gemma
Campbell, Peter J.
Forbes, Simon
Jia, Mingming
Jones, David
Knott, Henry
Kok, Chai Yin
Lau, King Wai
Leroy, Catherine
Lin, Meng-Lay
McBride, David J
Maddison, Mark
Maguire, Simon
McLay, Kirsten
Menzies, Andrew
Mironenko, Tatiana
Mulderrig, Lee
Mudie, Laura
O’Meara, Sarah
Pleasance, Erin
Rajasingham, Arjunan
Shepherd, Rebecca
Smith, Raffaella
Stebbings, Lucy
Stephens, Philip
Tang, Gurpreet
Tarpey, Patrick S
Turrell, Kelly
Dykema, Karl J.
Khoo, Sok Kean
Petillo, David
Wondergem, Bill
Anema, John
Kahnoski, Richard J.
Teh, Bin Tean
Stratton, Michael R.
Futreal, P. Andrew
Systematic sequencing of renal carcinoma reveals inactivation of histone modifying genes
title Systematic sequencing of renal carcinoma reveals inactivation of histone modifying genes
title_full Systematic sequencing of renal carcinoma reveals inactivation of histone modifying genes
title_fullStr Systematic sequencing of renal carcinoma reveals inactivation of histone modifying genes
title_full_unstemmed Systematic sequencing of renal carcinoma reveals inactivation of histone modifying genes
title_short Systematic sequencing of renal carcinoma reveals inactivation of histone modifying genes
title_sort systematic sequencing of renal carcinoma reveals inactivation of histone modifying genes
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2820242/
https://www.ncbi.nlm.nih.gov/pubmed/20054297
http://dx.doi.org/10.1038/nature08672
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