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Co-expression of mitosis-regulating genes contributes to malignant progression and prognosis in oligodendrogliomas

The clinical prognosis of patients with glioma is determined by tumor grades, but tumors of different subtypes with equal malignancy grade usually have different prognosis that is largely determined by genetic abnormalities. Oligodendrogliomas (ODs) are the second most common type of gliomas. In thi...

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Autores principales: Liu, Yanwei, Hu, Huimin, Zhang, Chuanbao, Wang, Haoyuan, Zhang, Wenlong, Wang, Zheng, Li, Mingyang, Zhang, Wei, Zhou, Dabiao, Jiang, Tao
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4741997/
https://www.ncbi.nlm.nih.gov/pubmed/26468983
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author Liu, Yanwei
Hu, Huimin
Zhang, Chuanbao
Wang, Haoyuan
Zhang, Wenlong
Wang, Zheng
Li, Mingyang
Zhang, Wei
Zhou, Dabiao
Jiang, Tao
author_facet Liu, Yanwei
Hu, Huimin
Zhang, Chuanbao
Wang, Haoyuan
Zhang, Wenlong
Wang, Zheng
Li, Mingyang
Zhang, Wei
Zhou, Dabiao
Jiang, Tao
author_sort Liu, Yanwei
collection PubMed
description The clinical prognosis of patients with glioma is determined by tumor grades, but tumors of different subtypes with equal malignancy grade usually have different prognosis that is largely determined by genetic abnormalities. Oligodendrogliomas (ODs) are the second most common type of gliomas. In this study, integrative analyses found that distribution of TCGA transcriptomic subtypes was associated with grade progression in ODs. To identify critical gene(s) associated with tumor grades and TCGA subtypes, we analyzed 34 normal brain tissue (NBT), 146 WHO grade II and 130 grade III ODs by microarray and RNA sequencing, and identified a co-expression network of six genes (AURKA, NDC80,CENPK, KIAA0101, TIMELESS and MELK) that was associated with tumor grades and TCGA subtypes as well as Ki-67 expression. Validation of the six genes was performed by qPCR in additional 28 ODs. Importantly, these genes also were validated in four high-grade recurrent gliomas and the initial lower-grade gliomas resected from the same patients. Finally, the RNA data on two genes with the highest discrimination potential (AURKA and NDC80) and Ki-67 were validated on an independent cohort (5 NBTs and 86 ODs) by immunohistochemistry. Knockdown of AURKA and NDC80 by siRNAs suppressed Ki-67 expression and proliferation of gliomas cells. Survival analysis showed that high expression of the six genes corporately indicated a poor survival outcome. Correlation and protein interaction analysis provided further evidence for this co-expression network. These data suggest that the co-expression of the six mitosis-regulating genes was associated with malignant progression and prognosis in ODs.
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spelling pubmed-47419972016-03-17 Co-expression of mitosis-regulating genes contributes to malignant progression and prognosis in oligodendrogliomas Liu, Yanwei Hu, Huimin Zhang, Chuanbao Wang, Haoyuan Zhang, Wenlong Wang, Zheng Li, Mingyang Zhang, Wei Zhou, Dabiao Jiang, Tao Oncotarget Research Paper The clinical prognosis of patients with glioma is determined by tumor grades, but tumors of different subtypes with equal malignancy grade usually have different prognosis that is largely determined by genetic abnormalities. Oligodendrogliomas (ODs) are the second most common type of gliomas. In this study, integrative analyses found that distribution of TCGA transcriptomic subtypes was associated with grade progression in ODs. To identify critical gene(s) associated with tumor grades and TCGA subtypes, we analyzed 34 normal brain tissue (NBT), 146 WHO grade II and 130 grade III ODs by microarray and RNA sequencing, and identified a co-expression network of six genes (AURKA, NDC80,CENPK, KIAA0101, TIMELESS and MELK) that was associated with tumor grades and TCGA subtypes as well as Ki-67 expression. Validation of the six genes was performed by qPCR in additional 28 ODs. Importantly, these genes also were validated in four high-grade recurrent gliomas and the initial lower-grade gliomas resected from the same patients. Finally, the RNA data on two genes with the highest discrimination potential (AURKA and NDC80) and Ki-67 were validated on an independent cohort (5 NBTs and 86 ODs) by immunohistochemistry. Knockdown of AURKA and NDC80 by siRNAs suppressed Ki-67 expression and proliferation of gliomas cells. Survival analysis showed that high expression of the six genes corporately indicated a poor survival outcome. Correlation and protein interaction analysis provided further evidence for this co-expression network. These data suggest that the co-expression of the six mitosis-regulating genes was associated with malignant progression and prognosis in ODs. Impact Journals LLC 2015-10-12 /pmc/articles/PMC4741997/ /pubmed/26468983 Text en Copyright: © 2015 Liu 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
Liu, Yanwei
Hu, Huimin
Zhang, Chuanbao
Wang, Haoyuan
Zhang, Wenlong
Wang, Zheng
Li, Mingyang
Zhang, Wei
Zhou, Dabiao
Jiang, Tao
Co-expression of mitosis-regulating genes contributes to malignant progression and prognosis in oligodendrogliomas
title Co-expression of mitosis-regulating genes contributes to malignant progression and prognosis in oligodendrogliomas
title_full Co-expression of mitosis-regulating genes contributes to malignant progression and prognosis in oligodendrogliomas
title_fullStr Co-expression of mitosis-regulating genes contributes to malignant progression and prognosis in oligodendrogliomas
title_full_unstemmed Co-expression of mitosis-regulating genes contributes to malignant progression and prognosis in oligodendrogliomas
title_short Co-expression of mitosis-regulating genes contributes to malignant progression and prognosis in oligodendrogliomas
title_sort co-expression of mitosis-regulating genes contributes to malignant progression and prognosis in oligodendrogliomas
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4741997/
https://www.ncbi.nlm.nih.gov/pubmed/26468983
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