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Combination genetic signature stratifies lower-grade gliomas better than histological grade

We studied if combination genetic signature potentially stratifies lower-grade gliomas better than histology by investigating 214 lower-grade gliomas for IDH1/2 and TERTp mutations, 1p/19q codeletion and EGFR amplification as to their impact on prognostication. Prognostic association of grading was...

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Autores principales: Chan, Aden Ka-Yin, Yao, Yu, Zhang, Zhenyu, Shi, Zhifeng, Chen, Liang, Chung, Nellie Yuk-Fei, Liu, Joseph Shu-Ming, Li, Kay Ka-Wai, Chan, Danny Tat-Ming, Poon, Wai Sang, Wang, Ying, Zhou, Liangfu, Ng, Ho-Keung
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4673237/
https://www.ncbi.nlm.nih.gov/pubmed/26369702
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author Chan, Aden Ka-Yin
Yao, Yu
Zhang, Zhenyu
Shi, Zhifeng
Chen, Liang
Chung, Nellie Yuk-Fei
Liu, Joseph Shu-Ming
Li, Kay Ka-Wai
Chan, Danny Tat-Ming
Poon, Wai Sang
Wang, Ying
Zhou, Liangfu
Ng, Ho-Keung
author_facet Chan, Aden Ka-Yin
Yao, Yu
Zhang, Zhenyu
Shi, Zhifeng
Chen, Liang
Chung, Nellie Yuk-Fei
Liu, Joseph Shu-Ming
Li, Kay Ka-Wai
Chan, Danny Tat-Ming
Poon, Wai Sang
Wang, Ying
Zhou, Liangfu
Ng, Ho-Keung
author_sort Chan, Aden Ka-Yin
collection PubMed
description We studied if combination genetic signature potentially stratifies lower-grade gliomas better than histology by investigating 214 lower-grade gliomas for IDH1/2 and TERTp mutations, 1p/19q codeletion and EGFR amplification as to their impact on prognostication. Prognostic association of grading was independent of other prognostic variables including age, histological type, IDH1/2, 1p/19q and TERTp status. No single marker, including IDH1/2, superseded grading in prognostication, indicating grading was still a very important tool. Prognosis was most favorable in 31.7% of patients with IDH1/2 mutation and either 1p/19q codeletion or TERTp mutation (IDHmut-OT), intermediate in 45.8% of patients with IDH1/2 mutation only (IDHmut) and 16.9% of patients without any of the alterations (IDHwt), and poorest in 5.6% of patients with wild-type IDH1/2 and either TERTp mutation or EGFR amplification (IDHwt-ET). Our results suggested not all IDH1/2 wild-type lower-grade gliomas are aggressive and additional biomarkers are required to identify glioblastoma-equivalent tumors. Multivariate analysis revealed independent prognostic values of grading and genetic signature. Grade II IDHwt-ET gliomas exhibited shorter survival than IDH1/2 mutated grade III gliomas, suggesting combination genetic signature potentially superseded grading in prognostication. In summary, biomarker-based stratification is useful in the diagnosis and prognostication of lower-grade gliomas, and should be used together with grading.
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spelling pubmed-46732372015-12-22 Combination genetic signature stratifies lower-grade gliomas better than histological grade Chan, Aden Ka-Yin Yao, Yu Zhang, Zhenyu Shi, Zhifeng Chen, Liang Chung, Nellie Yuk-Fei Liu, Joseph Shu-Ming Li, Kay Ka-Wai Chan, Danny Tat-Ming Poon, Wai Sang Wang, Ying Zhou, Liangfu Ng, Ho-Keung Oncotarget Research Paper: Pathology We studied if combination genetic signature potentially stratifies lower-grade gliomas better than histology by investigating 214 lower-grade gliomas for IDH1/2 and TERTp mutations, 1p/19q codeletion and EGFR amplification as to their impact on prognostication. Prognostic association of grading was independent of other prognostic variables including age, histological type, IDH1/2, 1p/19q and TERTp status. No single marker, including IDH1/2, superseded grading in prognostication, indicating grading was still a very important tool. Prognosis was most favorable in 31.7% of patients with IDH1/2 mutation and either 1p/19q codeletion or TERTp mutation (IDHmut-OT), intermediate in 45.8% of patients with IDH1/2 mutation only (IDHmut) and 16.9% of patients without any of the alterations (IDHwt), and poorest in 5.6% of patients with wild-type IDH1/2 and either TERTp mutation or EGFR amplification (IDHwt-ET). Our results suggested not all IDH1/2 wild-type lower-grade gliomas are aggressive and additional biomarkers are required to identify glioblastoma-equivalent tumors. Multivariate analysis revealed independent prognostic values of grading and genetic signature. Grade II IDHwt-ET gliomas exhibited shorter survival than IDH1/2 mutated grade III gliomas, suggesting combination genetic signature potentially superseded grading in prognostication. In summary, biomarker-based stratification is useful in the diagnosis and prognostication of lower-grade gliomas, and should be used together with grading. Impact Journals LLC 2015-08-11 /pmc/articles/PMC4673237/ /pubmed/26369702 Text en Copyright: © 2015 Chan et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper: Pathology
Chan, Aden Ka-Yin
Yao, Yu
Zhang, Zhenyu
Shi, Zhifeng
Chen, Liang
Chung, Nellie Yuk-Fei
Liu, Joseph Shu-Ming
Li, Kay Ka-Wai
Chan, Danny Tat-Ming
Poon, Wai Sang
Wang, Ying
Zhou, Liangfu
Ng, Ho-Keung
Combination genetic signature stratifies lower-grade gliomas better than histological grade
title Combination genetic signature stratifies lower-grade gliomas better than histological grade
title_full Combination genetic signature stratifies lower-grade gliomas better than histological grade
title_fullStr Combination genetic signature stratifies lower-grade gliomas better than histological grade
title_full_unstemmed Combination genetic signature stratifies lower-grade gliomas better than histological grade
title_short Combination genetic signature stratifies lower-grade gliomas better than histological grade
title_sort combination genetic signature stratifies lower-grade gliomas better than histological grade
topic Research Paper: Pathology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4673237/
https://www.ncbi.nlm.nih.gov/pubmed/26369702
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