Genomic profiling and prognostic factors of H3 K27M‐mutant spinal cord diffuse glioma

H3 K27‐altered diffuse midline glioma is a highly lethal pediatric‐type tumor without efficacious treatments. Recent findings have highlighted the heterogeneity among diffuse midline gliomas with different locations and ages. Compared to tumors located in the brain stem and thalamus, the molecular a...

Descripción completa

Detalles Bibliográficos
Autores principales: Chai, Rui‐Chao, Yan, Hao, An, Song‐Yuan, Pang, Bo, Chen, Hui‐Yuan, Mu, Quan‐Hua, Zhang, Ke‐Nan, Zhang, Yao‐Wu, Liu, Yu‐Qing, Liu, Xing, Zhao, Zheng, Jiang, Tao, Wang, Yong‐Zhi, Jia, Wen‐Qing
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2023
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10307522/
https://www.ncbi.nlm.nih.gov/pubmed/36751054
http://dx.doi.org/10.1111/bpa.13153
_version_ 1785066066997673984
author Chai, Rui‐Chao
Yan, Hao
An, Song‐Yuan
Pang, Bo
Chen, Hui‐Yuan
Mu, Quan‐Hua
Zhang, Ke‐Nan
Zhang, Yao‐Wu
Liu, Yu‐Qing
Liu, Xing
Zhao, Zheng
Jiang, Tao
Wang, Yong‐Zhi
Jia, Wen‐Qing
author_facet Chai, Rui‐Chao
Yan, Hao
An, Song‐Yuan
Pang, Bo
Chen, Hui‐Yuan
Mu, Quan‐Hua
Zhang, Ke‐Nan
Zhang, Yao‐Wu
Liu, Yu‐Qing
Liu, Xing
Zhao, Zheng
Jiang, Tao
Wang, Yong‐Zhi
Jia, Wen‐Qing
author_sort Chai, Rui‐Chao
collection PubMed
description H3 K27‐altered diffuse midline glioma is a highly lethal pediatric‐type tumor without efficacious treatments. Recent findings have highlighted the heterogeneity among diffuse midline gliomas with different locations and ages. Compared to tumors located in the brain stem and thalamus, the molecular and clinicopathological features of H3 K27‐altered spinal cord glioma are still largely elusive, thus hindering the accurate management of patients. Here we aimed to characterize the clinicopathological and molecular features of H3 K27M‐mutant spinal cord glioma in 77 consecutive cases. We found that the H3 K27M‐mutant spinal cord glioma, with a median age of 35 years old, had a significantly better prognosis than H3 K27M‐mutant brain tumors. We noticed a molecular heterogeneity of H3 K27M‐mutant spinal cord astrocytoma via targeted sequencing with 34 cases. TP53 mutation which occurred in 58.8% of cases is mutually exclusive with PPM1D (26%) and NF1 (44%) mutations. The TP53‐mutant cases had a significantly higher number of copy number variants (CNV) and a marginally higher proportion of pediatric patients (age at diagnosis <18 years old, p = 0.056). Cox regression and Kaplan–Meier curve analysis showed that the higher number of CNV events (≥3), chromosome (Chr) 9p deletion, Chr 10p deletion, ATRX mutation, CDK6 amplification, and retinoblastoma protein (RB) pathway alteration are associated with worse survival. Cox regression analysis with clinicopathological features showed that glioblastoma histological type and a high Ki‐67 index (>10%) are associated with a worse prognosis. Interestingly, the histological type, an independent prognostic factor in multivariate Cox regression, can also stratify molecular features of H3 K27M‐mutant spinal cord glioma, including the RB pathway, KRAS/PI3K pathway, and chromosome arms CNV. In conclusion, although all H3 K27M‐mutant spinal cord diffuse glioma were diagnosed as WHO Grade 4, the histological type, molecular features representing chromatin instability, and molecular alterations associated with accelerated cell proliferative activity should not be ignored in clinical management.
format Online
Article
Text
id pubmed-10307522
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher John Wiley and Sons Inc.
record_format MEDLINE/PubMed
spelling pubmed-103075222023-06-30 Genomic profiling and prognostic factors of H3 K27M‐mutant spinal cord diffuse glioma Chai, Rui‐Chao Yan, Hao An, Song‐Yuan Pang, Bo Chen, Hui‐Yuan Mu, Quan‐Hua Zhang, Ke‐Nan Zhang, Yao‐Wu Liu, Yu‐Qing Liu, Xing Zhao, Zheng Jiang, Tao Wang, Yong‐Zhi Jia, Wen‐Qing Brain Pathol Research Articles H3 K27‐altered diffuse midline glioma is a highly lethal pediatric‐type tumor without efficacious treatments. Recent findings have highlighted the heterogeneity among diffuse midline gliomas with different locations and ages. Compared to tumors located in the brain stem and thalamus, the molecular and clinicopathological features of H3 K27‐altered spinal cord glioma are still largely elusive, thus hindering the accurate management of patients. Here we aimed to characterize the clinicopathological and molecular features of H3 K27M‐mutant spinal cord glioma in 77 consecutive cases. We found that the H3 K27M‐mutant spinal cord glioma, with a median age of 35 years old, had a significantly better prognosis than H3 K27M‐mutant brain tumors. We noticed a molecular heterogeneity of H3 K27M‐mutant spinal cord astrocytoma via targeted sequencing with 34 cases. TP53 mutation which occurred in 58.8% of cases is mutually exclusive with PPM1D (26%) and NF1 (44%) mutations. The TP53‐mutant cases had a significantly higher number of copy number variants (CNV) and a marginally higher proportion of pediatric patients (age at diagnosis <18 years old, p = 0.056). Cox regression and Kaplan–Meier curve analysis showed that the higher number of CNV events (≥3), chromosome (Chr) 9p deletion, Chr 10p deletion, ATRX mutation, CDK6 amplification, and retinoblastoma protein (RB) pathway alteration are associated with worse survival. Cox regression analysis with clinicopathological features showed that glioblastoma histological type and a high Ki‐67 index (>10%) are associated with a worse prognosis. Interestingly, the histological type, an independent prognostic factor in multivariate Cox regression, can also stratify molecular features of H3 K27M‐mutant spinal cord glioma, including the RB pathway, KRAS/PI3K pathway, and chromosome arms CNV. In conclusion, although all H3 K27M‐mutant spinal cord diffuse glioma were diagnosed as WHO Grade 4, the histological type, molecular features representing chromatin instability, and molecular alterations associated with accelerated cell proliferative activity should not be ignored in clinical management. John Wiley and Sons Inc. 2023-02-07 /pmc/articles/PMC10307522/ /pubmed/36751054 http://dx.doi.org/10.1111/bpa.13153 Text en © 2023 The Authors. Brain Pathology published by John Wiley & Sons Ltd on behalf of International Society of Neuropathology. https://creativecommons.org/licenses/by-nc/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc/4.0/ (https://creativecommons.org/licenses/by-nc/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited and is not used for commercial purposes.
spellingShingle Research Articles
Chai, Rui‐Chao
Yan, Hao
An, Song‐Yuan
Pang, Bo
Chen, Hui‐Yuan
Mu, Quan‐Hua
Zhang, Ke‐Nan
Zhang, Yao‐Wu
Liu, Yu‐Qing
Liu, Xing
Zhao, Zheng
Jiang, Tao
Wang, Yong‐Zhi
Jia, Wen‐Qing
Genomic profiling and prognostic factors of H3 K27M‐mutant spinal cord diffuse glioma
title Genomic profiling and prognostic factors of H3 K27M‐mutant spinal cord diffuse glioma
title_full Genomic profiling and prognostic factors of H3 K27M‐mutant spinal cord diffuse glioma
title_fullStr Genomic profiling and prognostic factors of H3 K27M‐mutant spinal cord diffuse glioma
title_full_unstemmed Genomic profiling and prognostic factors of H3 K27M‐mutant spinal cord diffuse glioma
title_short Genomic profiling and prognostic factors of H3 K27M‐mutant spinal cord diffuse glioma
title_sort genomic profiling and prognostic factors of h3 k27m‐mutant spinal cord diffuse glioma
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10307522/
https://www.ncbi.nlm.nih.gov/pubmed/36751054
http://dx.doi.org/10.1111/bpa.13153
work_keys_str_mv AT chairuichao genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT yanhao genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT ansongyuan genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT pangbo genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT chenhuiyuan genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT muquanhua genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT zhangkenan genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT zhangyaowu genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT liuyuqing genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT liuxing genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT zhaozheng genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT jiangtao genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT wangyongzhi genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma
AT jiawenqing genomicprofilingandprognosticfactorsofh3k27mmutantspinalcorddiffuseglioma

Ejemplares similares