Polycomb group genes are targets of aberrant DNA methylation in renal cell carcinoma.
Michele Avissar-Whiting,Devin C. Koestler,E. Andres Houseman,Brock C. Christensen,Karl T. Kelsey,Carmen J. Marsit +5 more
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TL;DR: In this article, the authors defined profiles of DNA methylation in primary renal cell carcinomas (RCC) and assessed the association of these profiles with the expression of genes required for the establishment and maintenance of epigenetic marks.
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Abstract: The combined effects of genetic and epigenetic aberrations are well recognized as causal in tumorigenesis. Here, we defined profiles of DNA methylation in primary renal cell carcinomas (RCC) and assessed the association of these profiles with the expression of genes required for the establishment and maintenance of epigenetic marks. A bead-based methylation array platform was used to measure methylation of 1,413 CpG loci in ~800 cancer-associated genes and three methylation classes were derived by unsupervised clustering of tumors using recursively partitioned mixture modeling (RPMM). Quantitative RT-PCR was performed on all tumor samples to determine the expression of DNMT1, DNMT3B, VEZF1 and EZH2. Additionally, methylation at LINE-1 and AluYb8 repetitive elements was measured using bisulfite pyrosequencing. Associations between methylation class and tumor stage (p = 0.05), LINE-1 (p < 0.0001) and AluYb8 (p < 0.0001) methylation, as well as EZH2 expression (p < 0.0001) were noted following univariate analyses. A multinomial logistic regression model controlling for potential confounders revealed that AluYb8 (p < 0.003) methylation and EZH2 expression (p < 0.008) were significantly associated with methylation class membership. Because EZH2 is a member of the Polycomb repressive complex 2 (PRC2), we next analyzed the distribution of Polycomb group (PcG) targets among methylation classes derived by clustering the 1,413 array CpG loci using RPMM. PcG target genes were significantly enriched (p < 0.0001) in methylation classes with greater differential methylation between RCC and non-diseased kidney tissue. This work contributes to our understanding of how repressive marks on DNA and chromatin are dysregulated in carcinogenesis, knowledge that might aid the development of therapies or preventive strategies for human malignancies.
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Citations
Reduced H3K27me3 and DNA Hypomethylation Are Major Drivers of Gene Expression in K27M Mutant Pediatric High-Grade Gliomas
Sebastian Bender,Sebastian Bender,Yujie Tang,Anders Lindroth,Volker Hovestadt,David T.W. Jones,Marcel Kool,Marc Zapatka,Paul A. Northcott,Dominik Sturm,Wei Wang,Bernhard Radlwimmer,Jonas W. Højfeldt,Nathalene Truffaux,David Castel,Simone Schubert,Marina Ryzhova,Huriye Seker-Cin,Jan Gronych,Pascal-David Johann,Pascal-David Johann,Sebastian Stark,Sebastian Stark,Jochen Meyer,Jochen Meyer,Till Milde,Till Milde,Martin U. Schuhmann,Martin Ebinger,Camelia M. Monoranu,Anitha Ponnuswami,S. Chen,Chris Jones,Olaf Witt,Olaf Witt,V. Peter Collins,Andreas von Deimling,Andreas von Deimling,Nada Jabado,Stéphanie Puget,Jacques Grill,Kristian Helin,Andrey Korshunov,Andrey Korshunov,Peter Lichter,Michelle Monje,Christoph Plass,Yoon Jae Cho,Stefan M. Pfister,Stefan M. Pfister +49 more
TL;DR: It is shown that reduced H3K27me3 levels and DNA hypomethylation act in concert to activate gene expression in K27M mutant pHGGs, and it is demonstrated that this is caused by aberrant recruitment of the PRC2 complex to K 27M mutant H3.3.
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Circulating Tumor Cell Clustering Shapes DNA Methylation to Enable Metastasis Seeding.
Sofia Gkountela,Francesc Castro-Giner,Francesc Castro-Giner,Barbara Maria Szczerba,Marcus Vetter,Julia Landin,Ramona Scherrer,Ilona Krol,Manuel C. Scheidmann,Christian Beisel,Christian U. Stirnimann,Christian Kurzeder,Viola Heinzelmann-Schwarz,Christoph Rochlitz,Walter P. Weber,Nicola Aceto +15 more
TL;DR: The results link CTC clustering to specific changes in DNA methylation that promote stemness and metastasis and point to cluster-targeting compounds to suppress the spread of cancer.
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Widespread resetting of DNA methylation in glioblastoma-initiating cells suppresses malignant cellular behavior in a lineage-dependent manner
Stefan H. Stricker,Andrew Feber,Pär G. Engström,Helena Carén,Kathreena M Kurian,Yasuhiro Takashima,Yasuhiro Takashima,Colin Watts,Michael Way,Peter B. Dirks,Paul Bertone,Austin Smith,Austin Smith,Stephan Beck,Steven M. Pollard +14 more
TL;DR: Surprisingly, despite such global epigenetic reconfiguration, GiPSC-derived neural progenitors remained highly malignant upon xenotransplantation, suggesting that imposing an epigenome associated with an alternative developmental lineage can suppress malignant behavior.
Alternative Splicing of EZH2 pre-mRNA by SF3B3 Contributes to the Tumorigenic Potential of Renal Cancer
Ke Chen,Haibing Xiao,Jin Zeng,Gan Yu,Hui Zhou,Chunhua Huang,Weimin Yao,Wei Xiao,Junhui Hu,Wei Guan,Lily Wu,Jiaoti Huang,Qihong Huang,Hua Xu,Zhangqun Ye +14 more
TL;DR: SF3B3 as a key regulator of EZH2 pre-mRNA splicing and SF3B 3 may represent a novel prognostic factor and potential therapeutic target in ccRCC are suggested.
Peripheral blood DNA methylation profiles are indicative of head and neck squamous cell carcinoma: an epigenome-wide association study.
Scott M. Langevin,Devin C. Koestler,Brock C. Christensen,Rondi A. Butler,John K. Wiencke,Heather H. Nelson,E. Andres Houseman,Carmen J. Marsit,Karl T. Kelsey +8 more
TL;DR: A novel blood-based methylation profile that is indicative of HNSCC with a high degree of accuracy is identified and demonstrates the potential of DNA methylation measured in blood for development of non-invasive applications for detection of head and neck cancer.
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