The Somatic Genomic Landscape of Glioblastoma

McKenna, Aaron; Campos, Benito; Genovese, Giannicola; Shukla, Sachet A.; Meir, Erwin G. Van; Guha, Abhijit; Gibbs, Richard A.; Marra, Marco A.; Spellman, Paul T.; Weinstein, John N.; Benz, Christopher C.; Barnholtz‐Sloan, Jill S.; Barrett, Wendi; Ostrom, Quinn T.; Wolinsky, Yingli; Black, Keith L.; Bose, Bikash; Boulos, Paul T.; Boulos, Madgy; Brown, Jenn; Czerinski, Christine; Eppley, Matthew; Iacocca, Mary; Kempista, Thelma; Kitko, Teresa; Koyfman, Yakov; Rabeno, Brenda; Rastogi, Pawan; Sugarman, Michael C.; Swanson, Patricia; Yalamanchii, Kennedy; Otey, Ilana P.; Liu, Yingchun Spring; Xiao, Yonghong; Auman, J. Todd; Chen, Peng; Hadjipanayis, Angela; Lee, Eunjung; Lee, Semin; Park, Peter J.; Seidman, Jonathan G.; Yang, Lixing; Kucherlapati, Raju; Kalkanis, Steven N.; Mikkelsen, Tom; Poisson, Laila; Raghunathan, Aditya; Scarpace, Lisa; Bernard, Brady; Bressler, Ryan; Eakin, Andrea; Iype, Lisa; Kreisberg, Richard; Leinonen, Kalle; Reynolds, Sheila M.; Rovira, Hector; Thórsson, Vésteinn; Shmulevich, Ilya; Annala, Matti; Penny, Robert; Paulauskis, Joseph; Curley, Erin; Hatfield, Martha; Mallery, David; Morris, Scott; Shelton, Troy; Shelton, Candace; Sherman, Mark E.; Yena, Peggy; Cuppini, Lucia; DiMeco, Francesco; Eoli, Marica; Finocchiaro, Gaetano; Maderna, Emanuela; Pollo, Bianca; Saini, Marco; Balu, Saianand; Hoadley, Katherine A.; Li, Ling; Miller, C. Ryan; Shi, Yan; Topal, Michael D.; Wu, Junyuan; Dunn, Gavin P.; Giannini, Caterina; O’Neill, Brian Patrick; Aksoy, Bülent Arman; Antipin, Yevgeniy; Borsu, Laetitia; Berman, Samuel H.; Brennan, Cameron; Cerami, Ethan; Chakravarty, Debyani; Ciriello, Giovanni; Gao, Jianjiong; Groß, Benjamin; Jacobsen, Anders; Ladanyi, Marc; Lash, Alex E.; Liang, Yupu; Reva, Boris; Sander, Chris; Schultz, Nikolaus; Shen, Ronglai; Socci, Nicholas D.; Viale, Agnès; Ferguson, Martin L.; Chen, Qingrong; Demchok, John A.; Dillon, Laura A. L.; Shaw, Kenna; Sheth, Margi; Tarnuzzer, Roy; Wang, Zhining; Yang, Liming; Davidsen, Tanja M.; Guyer, Mark S.; Ozenberger, Bradley A.; Sofia, Heidi J.; Bergsten, Julie; Eckman, John; Harr, Jodi; Myers, Jerome; Smith, Christine; Tucker, Kelly J.; Winemiller, Cindy; Zach, Leigh Anne; Ljubimova, Julia Y.; Eley, Greg; Ayala, Brenda; Jensen, Mark A.; Kahn, A; Pihl, Todd; Pot, David; Wan, Yunhu; Eschbacher, Jennifer; Foltz, Greg; Hansen, Nathan; Hothi, Parvi; Lin, Biaoyang; Shah, Nameeta; Yoon, Jae-Geun; Lau, Ching C.; Berens, Michael E.; Ardlie, Kristin; Beroukhim, Rameen; Carter, Scott L.; Cherniack, Andrew D.; Noble, Mike; Cho, Juok; Cibulskis, Kristian; DiCara, Daniel; Frazer, Scott; Gabriel, Stacey; Gehlenborg, Nils; Gentry, Jeff; Heiman, David I.; Kim, Jaegil; Jiang, Rui; Lander, Eric S.; Lawrence, Michael S.; Lin, Pei; Mallard, Will; Meyerson, Matthew; Onofrio, Robert C.; Saksena, Gordon; Schumacher, Steve; Sougnez, Carrie; Stojanov, Petar; Tabak, Barbara; Voet, Doug; Zhang, Hailei; Zou, Lihua; Getz, Gad; Dees, Nathan N.; Li, Ding; Fulton, Lucinda L.; Fulton, Robert S.; Kanchi, Krishna-Latha; Mardis, Elaine R.; Wilson, Richard K.; Baylin, Stephen B.; Andrews, David W.; Harshyne, Larry A.; Cohen, Mark L.; Devine, Karen; Sloan, Andrew E.; VandenBerg, Scott R.; Berger, Mitchel S.; Prados, Michael D.; Carlin, Daniel E.; Craft, Brian; Ellrott, Kyle; Goldman, Mary; Goldstein, Theodore C.; Grifford, Mia; Haussler, David; Ma, Xiaotu; Ng, Sam; Salama, Sofie R.; Sanborn, J. Zachary; Stuart, Joshua M.; Swatloski, Teresa; Waltman, Peter; Zhu, Jing; Foss, Robin M.; Frentzen, Barbara; Friedman, William A.; McTiernan, Raquel G.; Yachnis, Anthony T.; Hayes, D. Neil; Perou, Charles M.; Zheng, Siyuan; Vegesna, Rahulsimham; Mao, Yong; Akbani, Rehan; Aldape, Kenneth; Bögler, Oliver; Fuller, Gregory N.; Liu, Wenbin; Liu, Yuexin; Lu, Yiling; Mills, Gordon B.; Protopopov, Alexei; Ren, Xiaojia; Sun, Youting; Wu, Chang-Jiun; Yung, W. K. Alfred; Zhang, Wei; Zhang, Jianhua; Chen, Ken; Weinstein, John N.; Chin, Lynda; Verhaak, Roel G.W.; Noushmehr, Houtan; Weisenberger, Daniel J.; Bootwalla, Moiz S.; Lai, Phillip H.; Triche, Timothy J.; Berg, David J. Van Den; Laird, Peter W.; Gutmann, David H.; Lehman, Norman L.; VanMeir, Erwin G.; Brat, Daniel J.; Olson, Jeffrey J.; Mastrogianakis, Gena M.; Devi, Narra S.; Zhang, Zhaobin; Bigner, Darell D.; Lipp, Eric; McLendon, Roger E.

doi:10.1016/j.cell.2013.09.034

Cited by 3,959 publications

(4,047 citation statements)

References 71 publications

Supporting

137

Mentioning

3,884

Contrasting

Unclassified

Order By: Relevance

“…P53 has been known to mutate in more than 50% of human cancers,13 including glioma. A previous study found that p53 signalling pathway was found to be dysregulated in 85.3% of glioma patients according to the TCGA (The Cancer Genome Atlas) data 14. Herein, we analysed signalling pathways closely related to glioma using Gene Set Enrichment Analysis (GSEA) to confirm the aberrant condition of p53 pathway.…”

Section: Introductionmentioning

confidence: 99%

Retracted: MircoRNA‐1275 promotes proliferation, invasion and migration of glioma cells via SERPINE1

Wang

Wen

et al. 2018

J Cellular Molecular Medi

View full text Add to dashboard Cite

This study was designed to explore the relationship between miR‐1275 and SERPINE1 and its effects on glioma cell proliferation, migration, invasion and apoptosis. Differentially expressed miRNAs and mRNAs in glioma tissues were screened out by bioinformatic analysis. Dual‐luciferase reporter gene assay was used to validate the targeted relationship between miR‐1275 and SERPINE1. qRT‐PCR was used to detect the expression of miR‐1275 and SERPINE1 in glioma tissues. The expressions of SERPINE1 and p53 pathway‐related proteins in glioma cells were detected by western blot. Glioma cell proliferation, apoptosis, migration and invasion were respectively detected by CCK‐8 assay, flow cytometry, wound healing assay and transwell assay. Tumour xenograft model was developed to study the influence of miR‐1275 and SERPINE1 on glioma growth in vivo. The results of microarray analysis, qRT‐PCR and western blot showed that miR‐1275 was low‐expressed while SERPINE1 was high‐expressed in glioma. Dual‐luciferase assay showed that miR‐1275 could bind to SERPINE1. Overexpression of miR‐1275 could promote the p53 pathway‐related proteins’ expression. Highly expressed miR‐1275 could repress the migration, proliferation and invasion of glioma cells while highly expressed SERPINE1 had inverse effects. Tumour xenograft showed that up‐regulated miR‐1275 or down‐regulated SERPINE1 could repress glioma growth in vivo. Up‐regulation of miR‐1275 activated p53 signalling pathway via regulating SERPINE1 and therefore suppressed glioma cell proliferation, invasion and migration, whereas promoted cell apoptosis.

show abstract

Section: Introductionmentioning

confidence: 99%

Retracted: MircoRNA‐1275 promotes proliferation, invasion and migration of glioma cells via SERPINE1

Wang

Wen

et al. 2018

J Cellular Molecular Medi

View full text Add to dashboard Cite

show abstract

“…The validation of their prognostic function by Kaplan‐Meier and Cox PH regression analyses revealed that age and the MGMT promoter methylation status were important prognostic markers that provide independent information. Primary GBM comprises 84.21% (265/304) of all adult GBM patients, and this ratio is lower than that reported in previous studies 1, 6. This discrepancy might be due to the classification of primary and secondary GBM based on the clinical history or IDH1/2 status in previous studies.…”

Section: Discussionmentioning

confidence: 56%

“…Among the five important variables identified in the random survival forest analysis, the MGMT promoter methylation status and TERT promoter mutation status are key molecular tumor markers of GBM 6. We analyzed the relationship between the MGMT promoter methylation status and the survival benefit associated with the TERT promoter mutation status.…”

Section: Resultsmentioning

confidence: 99%

“…Correspondingly, wild‐type IDH1/2 genotypes are considered robust biomarkers of primary GBM (<5%) 4, 5. Epigenetic alterations affecting the MGMT promoter methylation status and genetic mutations in the TERT promoter are considered molecular signatures of GBM,6 but few studies have investigated the prognostic significance of these molecular features in adult primary GBM. The diagnosis and monitoring of GBMs in neurosurgical practice are often accomplished through MRI visualization.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

The TERT promoter mutation status and MGMT promoter methylation status, combined with dichotomized MRI‐derived and clinical features, predict adult primary glioblastoma survival

et al. 2018

View full text Add to dashboard Cite

PurposeThis study aimed to integrate the TERT promoter mutation status, MGMT promoter methylation status, MRI‐derived features, and clinical features into a survival analysis model to better understand adult primary glioblastoma prognosis‐related markers.MethodA total of 304 adult glioblastoma samples collected after surgical resection were selected for retrospective analysis, and Sanger sequencing was performed to detect IDH and TERT promoter mutations. The methylation of the MGMT promoter was analyzed by pyrosequencing, and MRI‐derived and clinical features were dichotomized into easily acquired variables. Random survival forest analysis, Kaplan‐Meier analysis, Cox proportional hazard regression, and LASSO regression were performed for the survival analysis, and ROC analysis and Pearson's chi‐squared test were employed for the correlation analysis.ResultsWild‐type IDH was present in 89.8% of the adult glioblastoma samples, and TERT promoter mutations and MGMT promoter methylation were observed in 66.42% and 38.49% of all adult primary glioblastomas, respectively. Age and MGMT promoter methylation were identified as independent prognostic biomarkers, and the TERT promoter mutation status and MGMT promoter methylation status, when combined with other tumor‐related factors, generated several different survival subgroups. None of the factors investigated in this study predicted the MGMT promoter status, and MRI‐detected necrosis was positively associated with TERT promoter mutations.ConclusionMGMT promoter methylation and TERT promoter mutations, combined with MRI‐derived and clinical features, revealed different survival subgroups with distinct responses to current treatments, and this information increases the ability to predict the survival of adult primary glioblastoma patients. MRI‐detected necrosis often indicates the presence of TERT promoter mutations.

show abstract

“…Moreover, in a cohort of 154 patients with glioblastoma, KLRC3 has been founded mutated in 6% of the cases. By comparing the median survival of the patients included in the cohort, we founded a strong increase from 13.3 months for the patients without mutation to 25.4 months of survival for the patients having a mutated KLRC3 (from the TCGA analysis: The Cancer Genome Atlas) 16.…”

Section: Discussionmentioning

confidence: 99%

KLRC3, a Natural Killer receptor gene, is a key factor involved in glioblastoma tumourigenesis and aggressiveness

Cheray

Bessette

Lacroix

et al. 2016

J Cellular Molecular Medi

View full text Add to dashboard Cite

Glioblastoma is the most lethal brain tumour with a poor prognosis. Cancer stem cells (CSC) were proposed to be the most aggressive cells allowing brain tumour recurrence and aggressiveness. Current challenge is to determine CSC signature to characterize these cells and to develop new therapeutics. In a previous work, we achieved a screening of glycosylation‐related genes to characterize specific genes involved in CSC maintenance. Three genes named CHI3L1,KLRC3 and PRUNE2 were found overexpressed in glioblastoma undifferentiated cells (related to CSC) compared to the differentiated ones. The comparison of their roles suggest that KLRC3 gene coding for NKG2E, a protein initially identified in NK cells, is more important than both two other genes in glioblastomas aggressiveness. Indeed, KLRC3 silencing decreased self‐renewal capacity, invasion, proliferation, radioresistance and tumourigenicity of U87‐MG glioblastoma cell line. For the first time we report that KLRC3 gene expression is linked to glioblastoma aggressiveness and could be a new potential therapeutic target to attenuate glioblastoma.

show abstract

The Somatic Genomic Landscape of Glioblastoma

Cited by 3,959 publications

References 71 publications

Retracted: MircoRNA‐1275 promotes proliferation, invasion and migration of glioma cells via SERPINE1

Retracted: MircoRNA‐1275 promotes proliferation, invasion and migration of glioma cells via SERPINE1

The TERT promoter mutation status and MGMT promoter methylation status, combined with dichotomized MRI‐derived and clinical features, predict adult primary glioblastoma survival

KLRC3, a Natural Killer receptor gene, is a key factor involved in glioblastoma tumourigenesis and aggressiveness

Contact Info

Product

Resources

About