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Article: Molecular characterization of choroid plexus tumors reveals novel clinically relevant subgroups

TitleMolecular characterization of choroid plexus tumors reveals novel clinically relevant subgroups
Authors
Issue Date2015
Citation
Clinical Cancer Research, 2015, v. 21, n. 1, p. 184-192 How to Cite?
AbstractPurpose: To investigate molecular alterations in choroid plexus tumors (CPT) using a genome-wide high-throughput approach to identify diagnostic and prognostic signatures that will refine tumor stratification and guide therapeutic options. Experimental Design: One hundred CPTs were obtained from a multi-institutional tissue and clinical database. Copynumber (CN), DNA methylation, and gene expression signatures were assessed for 74, 36, and 40 samples, respectively. Molecular subgroups were correlated with clinical parameters and outcomes. Results: Unique molecular signatures distinguished choroid plexus carcinomas (CPC) from choroid plexus papillomas (CPP) and atypical choroid plexus papillomas (aCPP); however, no significantly distinct molecular alterations between CPPs and aCPPs were observed. Allele-specificCNanalysis of CPCs revealed two novel subgroups according to DNA content: hypodiploid and hyperdiploid CPCs. Hyperdiploid CPCs exhibited recurrent acquired uniparental disomy events. Somatic mutations in TP53 were observed in 60% of CPCs. Investigating the number of mutated copies of p53 per sample revealed a high-risk group of patients with CPC carrying two copies of mutant p53, who exhibited poor 5-year event-free (EFS) and overall survival (OS) compared with patients with CPC carrying one copy of mutant p53 (OS: 14.3%, 95% confidence interval, 0.71%-46.5% vs. 66.7%, 28.2%-87.8%, respectively, P = 0.04; EFS: 0% vs. 44.4%, 13.6%-71.9%, respectively, P = 0.03). CPPs and aCPPs exhibited favorable survival. Discussion: Our data demonstrate that differences in CN, gene expression, and DNA methylation signatures distinguish CPCs from CPPs and aCPPs; however, molecular similarities among the papillomas suggest that these two histologic subgroups are indeed a single molecular entity. A greater number of copies of mutated TP53 were significantly associated to increased tumor aggressiveness and a worse survival outcome in CPCs. Collectively, these findings will facilitate strati fied approaches to the clinical management of CPTs.
Persistent Identifierhttp://hdl.handle.net/10722/313967
ISSN
2023 Impact Factor: 10.0
2023 SCImago Journal Rankings: 4.623
ISI Accession Number ID

 

DC FieldValueLanguage
dc.contributor.authorMerino, Diana M.-
dc.contributor.authorShlien, Adam-
dc.contributor.authorVillani, Anita-
dc.contributor.authorPienkowska, Malgorzata-
dc.contributor.authorMack, Stephen-
dc.contributor.authorRamaswamy, Vijay-
dc.contributor.authorShih, David-
dc.contributor.authorTatevossian, Ruth-
dc.contributor.authorNovokmet, Ana-
dc.contributor.authorChoufani, Sanaa-
dc.contributor.authorDvir, Rina-
dc.contributor.authorBen-Arush, Myran-
dc.contributor.authorHarris, Brent T.-
dc.contributor.authorHwang, Eugene I.-
dc.contributor.authorLulla, Rishi-
dc.contributor.authorPfister, Stefan M.-
dc.contributor.authorAchatz, Maria Isabel-
dc.contributor.authorJabado, Nada-
dc.contributor.authorFinlay, Jonathan L.-
dc.contributor.authorWeksberg, Rosanna-
dc.contributor.authorBouffet, Eric-
dc.contributor.authorHawkins, Cynthia-
dc.contributor.authorTaylor, Michael D.-
dc.contributor.authorTabori, Uri-
dc.contributor.authorEllison, David W.-
dc.contributor.authorGilbertson, Richard J.-
dc.contributor.authorMalkin, David-
dc.date.accessioned2022-07-06T11:28:38Z-
dc.date.available2022-07-06T11:28:38Z-
dc.date.issued2015-
dc.identifier.citationClinical Cancer Research, 2015, v. 21, n. 1, p. 184-192-
dc.identifier.issn1078-0432-
dc.identifier.urihttp://hdl.handle.net/10722/313967-
dc.description.abstractPurpose: To investigate molecular alterations in choroid plexus tumors (CPT) using a genome-wide high-throughput approach to identify diagnostic and prognostic signatures that will refine tumor stratification and guide therapeutic options. Experimental Design: One hundred CPTs were obtained from a multi-institutional tissue and clinical database. Copynumber (CN), DNA methylation, and gene expression signatures were assessed for 74, 36, and 40 samples, respectively. Molecular subgroups were correlated with clinical parameters and outcomes. Results: Unique molecular signatures distinguished choroid plexus carcinomas (CPC) from choroid plexus papillomas (CPP) and atypical choroid plexus papillomas (aCPP); however, no significantly distinct molecular alterations between CPPs and aCPPs were observed. Allele-specificCNanalysis of CPCs revealed two novel subgroups according to DNA content: hypodiploid and hyperdiploid CPCs. Hyperdiploid CPCs exhibited recurrent acquired uniparental disomy events. Somatic mutations in TP53 were observed in 60% of CPCs. Investigating the number of mutated copies of p53 per sample revealed a high-risk group of patients with CPC carrying two copies of mutant p53, who exhibited poor 5-year event-free (EFS) and overall survival (OS) compared with patients with CPC carrying one copy of mutant p53 (OS: 14.3%, 95% confidence interval, 0.71%-46.5% vs. 66.7%, 28.2%-87.8%, respectively, P = 0.04; EFS: 0% vs. 44.4%, 13.6%-71.9%, respectively, P = 0.03). CPPs and aCPPs exhibited favorable survival. Discussion: Our data demonstrate that differences in CN, gene expression, and DNA methylation signatures distinguish CPCs from CPPs and aCPPs; however, molecular similarities among the papillomas suggest that these two histologic subgroups are indeed a single molecular entity. A greater number of copies of mutated TP53 were significantly associated to increased tumor aggressiveness and a worse survival outcome in CPCs. Collectively, these findings will facilitate strati fied approaches to the clinical management of CPTs.-
dc.languageeng-
dc.relation.ispartofClinical Cancer Research-
dc.titleMolecular characterization of choroid plexus tumors reveals novel clinically relevant subgroups-
dc.typeArticle-
dc.description.naturelink_to_subscribed_fulltext-
dc.identifier.doi10.1158/1078-0432.CCR-14-1324-
dc.identifier.pmid25336695-
dc.identifier.scopuseid_2-s2.0-84920664265-
dc.identifier.volume21-
dc.identifier.issue1-
dc.identifier.spage184-
dc.identifier.epage192-
dc.identifier.eissn1557-3265-
dc.identifier.isiWOS:000347462600023-

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