Chromosome copy number changes carry prognostic information independent of KIT/PDGFRA point mutations in gastrointestinal stromal tumors

Chromosome copy number changes carry prognostic information independent of KIT/PDGFRA point mutations in gastrointestinal stromal tumors

<p>Abstract</p> <p>Background</p> <p>Oncogenic point mutations in <it>KIT </it>or <it>PDGFRA </it>are recognized as the primary events responsible for the pathogenesis of most gastrointestinal stromal tumors (GIST), but additional genomic alterat...

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Main Authors: Lopes Paula, Santos Lúcio, Dinis José, Soares Marta, Santos Catarina, Mesquita Bárbara, Pinheiro Manuela, Pinto Carla, Vieira Joana, Ribeiro Franclim R, Veiga Isabel, Silva Mara, Afonso Mariana, Lopes Carlos, Teixeira Manuel R
Format: Article
Language:English
Published: BMC 2010-05-01
Series:BMC Medicine
Online Access:http://www.biomedcentral.com/1741-7015/8/26
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spelling doaj-ba31b7e8632a4636914a31fe8af085ee2020-11-24T21:20:19ZengBMCBMC Medicine1741-70152010-05-01812610.1186/1741-7015-8-26Chromosome copy number changes carry prognostic information independent of KIT/PDGFRA point mutations in gastrointestinal stromal tumorsLopes PaulaSantos LúcioDinis JoséSoares MartaSantos CatarinaMesquita BárbaraPinheiro ManuelaPinto CarlaVieira JoanaRibeiro Franclim RVeiga IsabelSilva MaraAfonso MarianaLopes CarlosTeixeira Manuel R<p>Abstract</p> <p>Background</p> <p>Oncogenic point mutations in <it>KIT </it>or <it>PDGFRA </it>are recognized as the primary events responsible for the pathogenesis of most gastrointestinal stromal tumors (GIST), but additional genomic alterations are frequent and presumably required for tumor progression. The relative contribution of such alterations for the biology and clinical behavior of GIST, however, remains elusive.</p> <p>Methods</p> <p>In the present study, somatic mutations in <it>KIT </it>and <it>PDGFRA </it>were evaluated by direct sequencing analysis in a consecutive series of 80 GIST patients. For a subset of 29 tumors, comparative genomic hybridization was additionally used to screen for chromosome copy number aberrations. Genotype and genomic findings were cross-tabulated and compared with available clinical and follow-up data.</p> <p>Results</p> <p>We report an overall mutation frequency of 87.5%, with 76.25% of the tumors showing alterations in <it>KIT </it>and 11.25% in <it>PDGFRA</it>. Secondary <it>KIT </it>mutations were additionally found in two of four samples obtained after imatinib treatment. Chromosomal imbalances were detected in 25 out of 29 tumors (86%), namely losses at 14q (88% of abnormal cases), 22q (44%), 1p (44%), and 15q (36%), and gains at 1q (16%) and 12q (20%). In addition to clinico-pathological high-risk groups, patients with <it>KIT </it>mutations, genomic complexity, genomic gains and deletions at either 1p or 22q showed a significantly shorter disease-free survival. Furthermore, genomic complexity was the best predictor of disease progression in multivariate analysis.</p> <p>Conclusions</p> <p>In addition to <it>KIT/PDGFRA </it>mutational status, our findings indicate that secondary chromosomal changes contribute significantly to tumor development and progression of GIST and that genomic complexity carries independent prognostic value that complements clinico-pathological and genotype information.</p> http://www.biomedcentral.com/1741-7015/8/26
collection DOAJ
language English
format Article
sources DOAJ
author Lopes Paula
Santos Lúcio
Dinis José
Soares Marta
Santos Catarina
Mesquita Bárbara
Pinheiro Manuela
Pinto Carla
Vieira Joana
Ribeiro Franclim R
Veiga Isabel
Silva Mara
Afonso Mariana
Lopes Carlos
Teixeira Manuel R
spellingShingle Lopes Paula
Santos Lúcio
Dinis José
Soares Marta
Santos Catarina
Mesquita Bárbara
Pinheiro Manuela
Pinto Carla
Vieira Joana
Ribeiro Franclim R
Veiga Isabel
Silva Mara
Afonso Mariana
Lopes Carlos
Teixeira Manuel R
Chromosome copy number changes carry prognostic information independent of KIT/PDGFRA point mutations in gastrointestinal stromal tumors
BMC Medicine
author_facet Lopes Paula
Santos Lúcio
Dinis José
Soares Marta
Santos Catarina
Mesquita Bárbara
Pinheiro Manuela
Pinto Carla
Vieira Joana
Ribeiro Franclim R
Veiga Isabel
Silva Mara
Afonso Mariana
Lopes Carlos
Teixeira Manuel R
author_sort Lopes Paula
title Chromosome copy number changes carry prognostic information independent of KIT/PDGFRA point mutations in gastrointestinal stromal tumors
title_short Chromosome copy number changes carry prognostic information independent of KIT/PDGFRA point mutations in gastrointestinal stromal tumors
title_full Chromosome copy number changes carry prognostic information independent of KIT/PDGFRA point mutations in gastrointestinal stromal tumors
title_fullStr Chromosome copy number changes carry prognostic information independent of KIT/PDGFRA point mutations in gastrointestinal stromal tumors
title_full_unstemmed Chromosome copy number changes carry prognostic information independent of KIT/PDGFRA point mutations in gastrointestinal stromal tumors
title_sort chromosome copy number changes carry prognostic information independent of kit/pdgfra point mutations in gastrointestinal stromal tumors
publisher BMC
series BMC Medicine
issn 1741-7015
publishDate 2010-05-01
description <p>Abstract</p> <p>Background</p> <p>Oncogenic point mutations in <it>KIT </it>or <it>PDGFRA </it>are recognized as the primary events responsible for the pathogenesis of most gastrointestinal stromal tumors (GIST), but additional genomic alterations are frequent and presumably required for tumor progression. The relative contribution of such alterations for the biology and clinical behavior of GIST, however, remains elusive.</p> <p>Methods</p> <p>In the present study, somatic mutations in <it>KIT </it>and <it>PDGFRA </it>were evaluated by direct sequencing analysis in a consecutive series of 80 GIST patients. For a subset of 29 tumors, comparative genomic hybridization was additionally used to screen for chromosome copy number aberrations. Genotype and genomic findings were cross-tabulated and compared with available clinical and follow-up data.</p> <p>Results</p> <p>We report an overall mutation frequency of 87.5%, with 76.25% of the tumors showing alterations in <it>KIT </it>and 11.25% in <it>PDGFRA</it>. Secondary <it>KIT </it>mutations were additionally found in two of four samples obtained after imatinib treatment. Chromosomal imbalances were detected in 25 out of 29 tumors (86%), namely losses at 14q (88% of abnormal cases), 22q (44%), 1p (44%), and 15q (36%), and gains at 1q (16%) and 12q (20%). In addition to clinico-pathological high-risk groups, patients with <it>KIT </it>mutations, genomic complexity, genomic gains and deletions at either 1p or 22q showed a significantly shorter disease-free survival. Furthermore, genomic complexity was the best predictor of disease progression in multivariate analysis.</p> <p>Conclusions</p> <p>In addition to <it>KIT/PDGFRA </it>mutational status, our findings indicate that secondary chromosomal changes contribute significantly to tumor development and progression of GIST and that genomic complexity carries independent prognostic value that complements clinico-pathological and genotype information.</p>
url http://www.biomedcentral.com/1741-7015/8/26
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