Durable tumor regression in genetically altered malignant rhabdoid tumors by inhibition of methyltransferase EZH2

Knutson, Sarah K.; Warholic, Natalie M.; Wigle, Tim J.; Klaus, Christine; Allain, Christina J.; Raimondi, Alejandra; Scott, Margaret Porter; Chesworth, Richard; Moyer, Mikel P.; Copeland, Robert A.; Richon, Victoria M.; Pollock, Roy M.; Kuntz, Kevin W.; Keilhack, Heike

doi:10.1073/pnas.1303800110

Cited by 657 publications

(626 citation statements)

References 23 publications

(28 reference statements)

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“…A subset of these tumours with inactivated SMARCB1 are thought to be dependent on the catalytic activity of EZH2 and in xenograft models, were shown to be sensitive to treatment with the potent and selective EZH2 inhibitor, EPZ6438 (Ref. 44). …”

Section: Ezh2mentioning

confidence: 99%

Chromatin proteins and modifications as drug targets

Helin

Dhanak

2013

Nature

388

344

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Section: Ezh2mentioning

confidence: 99%

Chromatin proteins and modifications as drug targets

Helin

Dhanak

2013

Nature

388

344

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“…59 Finally, recent evidence suggests that EZH2 may also have a role in rhabdoid tumors. 63,88 Inactivation of the chromatin remodeler SWI/SNF complex component SNF5 is highly prevalent in this disease. Targeted disruption of EZH2 also strongly impairs ATRT cell growth, suppresses tumor cell self-renewal, induces apoptosis, and potently sensitizes these cells to radiation.…”

Section: Kmts and Prmtsmentioning

confidence: 99%

“…As the administered dose of compound correlates with reduction in H3K27me3 levels in tumor tissue and of tumor growth, the clinical use of such inhibitors for cancers in which EZH2 is genetically altered is relevant. 88,89 Interestingly, Kim and colleagues discovered that EZH2 enhances STAT3 activation by trimethylating lysine180 in STAT3, and it does so preferentially in glioma stem-like cells. 90 The use of the EZH2 inhibitor 3-deazaneplanocin A (DZNep) 91,92 and a highly selective EZH2 inhibitor GSK126 93 decreases STAT3 activation in glioma stem-like cells.…”

Section: Kmts and Prmtsmentioning

confidence: 99%

Epigenetic modification in chromatin machinery and its deregulation in pediatric brain tumors: Insight into epigenetic therapies

Maury

Hashizume

2017

Epigenetics

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Malignancies are characterized by the reprogramming of epigenetic patterns. This reprogramming includes gains or losses in DNA methylation and disruption of normal patterns of covalent histone modifications, which are associated with changes in chromatin remodeling processes. This review will focus on the mechanisms underlying this reprogramming and, specifically, on the role of histone modification in chromatin machinery and the modifications in epigenetic processes occurring in brain cancer, with a specific focus on epigenetic therapies for pediatric brain tumors.

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“…Most importantly, EZH2 overexpression in various types of cancers has been linked to oncogenesis, partly via H3K27me3 in promoters of specific tumor suppressor genes, and thus causes gene silencing (31). Targeting EZH2 is believed to be a promising strategy for cancer therapy (32,33).…”

mentioning

confidence: 99%

O-GlcNAcylation regulates EZH2 protein stability and function

Chu

Yeh

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

196

206

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O-linked N-acetylglucosamine (GlcNAc) transferase (OGT) is the only known enzyme that catalyzes the O-GlcNAcylation of proteins at the Ser or Thr side chain hydroxyl group. OGT participates in transcriptional and epigenetic regulation, and dysregulation of OGT has been implicated in diseases such as cancer. However, the underlying mechanism is largely unknown. Here we show that OGT is required for the trimethylation of histone 3 at K27 to form the product H3K27me3, a process catalyzed by the histone methyltransferase enhancer of zeste homolog 2 (EZH2) in the polycomb repressive complex 2 (PRC2). H3K27me3 is one of the most important histone modifications to mark the transcriptionally silenced chromatin. We found that the level of H3K27me3, but not other H3 methylation products, was greatly reduced upon OGT depletion. OGT knockdown specifically down-regulated the protein stability of EZH2, without altering the levels of H3K27 demethylases UTX and JMJD3, and disrupted the integrity of the PRC2 complex. Furthermore, the interaction of OGT and EZH2/PRC2 was detected by coimmunoprecipitation and cosedimentation experiments. Importantly, we identified that serine 75 is the site for EZH2 OGlcNAcylation, and the EZH2 mutant S75A exhibited reduction in stability. Finally, microarray and ChIP analysis have characterized a specific subset of potential tumor suppressor genes subject to repression via the OGT-EZH2 axis. Together these results indicate that OGT-mediated O-GlcNAcylation at S75 stabilizes EZH2 and hence facilitates the formation of H3K27me3. The study not only uncovers a functional posttranslational modification of EZH2 but also reveals a unique epigenetic role of OGT in regulating histone methylation.

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Durable tumor regression in genetically altered malignant rhabdoid tumors by inhibition of methyltransferase EZH2

Cited by 657 publications

References 23 publications

Chromatin proteins and modifications as drug targets

Chromatin proteins and modifications as drug targets

Epigenetic modification in chromatin machinery and its deregulation in pediatric brain tumors: Insight into epigenetic therapies

O-GlcNAcylation regulates EZH2 protein stability and function

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