Dynamic reprogramming of DNA methylation in SETD2-deregulated renal cell carcinoma

Rochelle L. Tiedemann; Ryan A. Hlady; Paul D. Hanavan; Douglas F. Lake; Raoul Tibes; Jeong Heon Lee; Jeong Hyeon Choi; Thai H. Ho; Keith D. Robertson

doi:10.18632/oncotarget.6481

Dynamic reprogramming of DNA methylation in SETD2-deregulated renal cell carcinoma

Rochelle L. Tiedemann, Ryan A. Hlady, Paul D. Hanavan, Douglas F. Lake, Raoul Tibes, Jeong Heon Lee, Jeong Hyeon Choi, Thai H. Ho, Keith D. Robertson

Research output: Contribution to journal › Article › peer-review

30 Scopus citations

Abstract

Clear cell renal cell carcinomas (ccRCCs) harbor frequent mutations in epigenetic modifiers including SETD2, the H3K36me3 writer. We profiled DNA methylation (5mC) across the genome in cell line-based models of SETD2 inactivation and SETD2 mutant primary tumors because 5mC has been linked to H3K36me3 and is therapeutically targetable. SETD2 depleted cell line models (long-term and acute) exhibited a DNA hypermethylation phenotype coinciding with ectopic gains in H3K36me3 centered across intergenic regions adjacent to low expressing genes, which became upregulated upon dysregulation of the epigenome. Poised enhancers of developmental genes were prominent hypermethylation targets. SETD2 mutant primary ccRCCs, papillary renal cell carcinomas, and lung adenocarcinomas all demonstrated a DNA hypermethylation phenotype that segregated tumors by SETD2 genotype and advanced grade. These findings collectively demonstrate that SETD2 mutations drive tumorigenesis by coordinated disruption of the epigenome and transcriptome, and they have important implications for future therapeutic strategies targeting chromatin regulator mutant tumors.

Original language	English (US)
Pages (from-to)	1927-1946
Number of pages	20
Journal	Oncotarget
Volume	7
Issue number	2
DOIs	https://doi.org/10.18632/oncotarget.6481
State	Published - 2016

Keywords

DNA methylation
Epigenetics
Histone methylation
Renal cell cancer
SETD2

ASJC Scopus subject areas

Oncology

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10.18632/oncotarget.6481

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title = "Dynamic reprogramming of DNA methylation in SETD2-deregulated renal cell carcinoma",

abstract = "Clear cell renal cell carcinomas (ccRCCs) harbor frequent mutations in epigenetic modifiers including SETD2, the H3K36me3 writer. We profiled DNA methylation (5mC) across the genome in cell line-based models of SETD2 inactivation and SETD2 mutant primary tumors because 5mC has been linked to H3K36me3 and is therapeutically targetable. SETD2 depleted cell line models (long-term and acute) exhibited a DNA hypermethylation phenotype coinciding with ectopic gains in H3K36me3 centered across intergenic regions adjacent to low expressing genes, which became upregulated upon dysregulation of the epigenome. Poised enhancers of developmental genes were prominent hypermethylation targets. SETD2 mutant primary ccRCCs, papillary renal cell carcinomas, and lung adenocarcinomas all demonstrated a DNA hypermethylation phenotype that segregated tumors by SETD2 genotype and advanced grade. These findings collectively demonstrate that SETD2 mutations drive tumorigenesis by coordinated disruption of the epigenome and transcriptome, and they have important implications for future therapeutic strategies targeting chromatin regulator mutant tumors.",

keywords = "DNA methylation, Epigenetics, Histone methylation, Renal cell cancer, SETD2",

author = "Tiedemann, {Rochelle L.} and Hlady, {Ryan A.} and Hanavan, {Paul D.} and Lake, {Douglas F.} and Raoul Tibes and Lee, {Jeong Heon} and Choi, {Jeong Hyeon} and Ho, {Thai H.} and Robertson, {Keith D.}",

note = "Funding Information: RLT is supported by NIH grant F31 CA171727. THH is supported by funding from the ASCO Young Investigator Award from the Kidney Cancer Association, NIH grant K12 CA90628, Gerstner Family Career Development Award, and a Kathryn H. and Roger Penske Career Development Award to Support Medical Research. KDR is supported by NIH grants R01 AA019976 and R01 CA114229, the Mayo Clinic Cancer Center, and the Mayo Clinic Center for Individualized Medicine.",

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doi = "10.18632/oncotarget.6481",

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AU - Tiedemann, Rochelle L.

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AU - Lake, Douglas F.

AU - Tibes, Raoul

AU - Lee, Jeong Heon

AU - Choi, Jeong Hyeon

AU - Ho, Thai H.

AU - Robertson, Keith D.

N1 - Funding Information: RLT is supported by NIH grant F31 CA171727. THH is supported by funding from the ASCO Young Investigator Award from the Kidney Cancer Association, NIH grant K12 CA90628, Gerstner Family Career Development Award, and a Kathryn H. and Roger Penske Career Development Award to Support Medical Research. KDR is supported by NIH grants R01 AA019976 and R01 CA114229, the Mayo Clinic Cancer Center, and the Mayo Clinic Center for Individualized Medicine.

PY - 2016

Y1 - 2016

N2 - Clear cell renal cell carcinomas (ccRCCs) harbor frequent mutations in epigenetic modifiers including SETD2, the H3K36me3 writer. We profiled DNA methylation (5mC) across the genome in cell line-based models of SETD2 inactivation and SETD2 mutant primary tumors because 5mC has been linked to H3K36me3 and is therapeutically targetable. SETD2 depleted cell line models (long-term and acute) exhibited a DNA hypermethylation phenotype coinciding with ectopic gains in H3K36me3 centered across intergenic regions adjacent to low expressing genes, which became upregulated upon dysregulation of the epigenome. Poised enhancers of developmental genes were prominent hypermethylation targets. SETD2 mutant primary ccRCCs, papillary renal cell carcinomas, and lung adenocarcinomas all demonstrated a DNA hypermethylation phenotype that segregated tumors by SETD2 genotype and advanced grade. These findings collectively demonstrate that SETD2 mutations drive tumorigenesis by coordinated disruption of the epigenome and transcriptome, and they have important implications for future therapeutic strategies targeting chromatin regulator mutant tumors.

AB - Clear cell renal cell carcinomas (ccRCCs) harbor frequent mutations in epigenetic modifiers including SETD2, the H3K36me3 writer. We profiled DNA methylation (5mC) across the genome in cell line-based models of SETD2 inactivation and SETD2 mutant primary tumors because 5mC has been linked to H3K36me3 and is therapeutically targetable. SETD2 depleted cell line models (long-term and acute) exhibited a DNA hypermethylation phenotype coinciding with ectopic gains in H3K36me3 centered across intergenic regions adjacent to low expressing genes, which became upregulated upon dysregulation of the epigenome. Poised enhancers of developmental genes were prominent hypermethylation targets. SETD2 mutant primary ccRCCs, papillary renal cell carcinomas, and lung adenocarcinomas all demonstrated a DNA hypermethylation phenotype that segregated tumors by SETD2 genotype and advanced grade. These findings collectively demonstrate that SETD2 mutations drive tumorigenesis by coordinated disruption of the epigenome and transcriptome, and they have important implications for future therapeutic strategies targeting chromatin regulator mutant tumors.

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Dynamic reprogramming of DNA methylation in SETD2-deregulated renal cell carcinoma

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