JHDM1B/FBXL10 is a nucleolar protein that represses transcription of ribosomal RNA genes

Frescas, David; Guardavaccaro, Daniele; Bassermann, Florian; Koyama‐Nasu, Ryo; Pagano, Michele

doi:10.1038/nature06255

Cited by 250 publications

(262 citation statements)

References 30 publications

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“…F-box proteins function as components of SCF-type E3 ubiquitin ligase complexes and may participate in co-repressor complexes (Gearhart et al 2006). The presence of a histone demethylase activity in FBXL10 was shown to be important for regulation of cell senescence and transcription of rRNAs (Jin et al 2004, Takeuchi et al 2006, Frescas et al 2007, He et al 2008, Pfau et al 2008, Yamagishi et al 2008. In our experiments, truncated versions of FBXL10 gene were recovered lacking the 5 0 -terminal part encoding the demethylase domain.…”

Section: Discussionmentioning

confidence: 76%

Selective recruitment of breast cancer anti-estrogen resistance genes and relevance for breast cancer progression and tamoxifen therapy response

Agthoven¹,

Sieuwerts²,

Meijer³

et al. 2010

Endocrine-Related Cancer

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Although endocrine treatment of breast cancer is effective and common practice, in advanced disease the development of resistance is nearly inevitable. To get more insight into individual genes that account for resistance against hormonal agents, we have executed functional genetic screens and subsequently evaluated the clinical relevance of several identified genes with respect to tumor aggressiveness and tamoxifen resistance in estrogen receptor-positive patients. Estrogen-dependent human breast cancer cells were transduced with different retroviral cDNA expression libraries and subjected to selective cultures with various anti-estrogens. From a total of 264 resistant cell clones, 132 different genes were recovered by PCR. By applying stringent selection criteria, we identified 15 breast cancer anti-estrogen resistance (BCAR) genes individually yielding resistance. BCAR genes were recovered with differential frequencies for the diverse culture conditions and anti-estrogen drugs. Analysis of the relation of BCAR genes (EIF1, FBXL10, HRAS, NRG1, PDGFRA, PDGFRB, RAD21, and RAF1) with tamoxifen treatment in patients with advanced disease showed significant association with clinical benefit and progression-free survival for EIF1 and PDGFRA mRNA levels. Furthermore, PDGFRA and HRAS mRNA levels were significantly associated with tumor aggressiveness in lymph node-negative patients who had not received adjuvant systemic therapy. In conclusion, our functional genetic screens showed that BCAR genes differ in their ability to confer resistance towards distinct antiestrogens. Based on the clinical relevance of several BCAR genes, further studies are warranted to characterize the underlying mechanisms, which may ultimately lead to the development of novel treatments and more individualized management of breast cancer patients.

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Section: Discussionmentioning

confidence: 76%

Selective recruitment of breast cancer anti-estrogen resistance genes and relevance for breast cancer progression and tamoxifen therapy response

Agthoven¹,

Sieuwerts²,

Meijer³

et al. 2010

Endocrine-Related Cancer

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“…Mutations that inactivate the tumor-suppressive activities of RB or p53 can result in aberrant upregulation of essential components of protein synthesis machinery and increase ribosome biogenesis, further leading to enhanced mRNA translation rates (28). JHDM1A and JHDM1B directly bind to rDNA promoter and repress the transcription of rRNA genes through epigenetic mechanisms (37,38). Moreover, some zinc finger proteins such as ZFP37, ZNF274, and JAZ are located and function in the nucleolus (39)(40)(41).…”

Section: Discussionmentioning

confidence: 99%

A Novel 19q13 Nucleolar Zinc Finger Protein Suppresses Tumor Cell Growth through Inhibiting Ribosome Biogenesis and Inducing Apoptosis but Is Frequently Silenced in Multiple Carcinomas

Cheng

Liang

Geng

et al. 2012

Molecular Cancer Research

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Epigenetic disruption of tumor suppressor genes is frequently involved in tumorigenesis. We identified a novel 19q13 KRAB domain-containing zinc finger protein, ZNF545/ZFP82, broadly expressed in normal tissues but downregulated in multiple tumor cell lines. The ZNF545 promoter contains a CpG island, which is frequently methylated in cell lines. The transcriptional silencing of ZNF545 could be reversed by pharmacologic or genetic demethylation, indicating direct epigenetic silencing. ZNF545 was also frequently methylated in multiple primary tumors of nasopharyngeal, esophageal, lung, gastric, colon, and breast, but rarely in normal epithelial tissues and paired normal tissues. ZNF545 is located in the nucleus and mainly sequestered in nucleoli, functioning as a repressor. ZNF545 is able to repress NF-kB and AP-1 signaling pathways, whereas ectopic expression of ZNF545 in silenced tumor cells significantly inhibited their growth and induced apoptosis. Functional studies showed that ZNF545 was involved in ribosome biogenesis through inhibiting the activity of rDNA promoter and decreasing cellular protein translation efficiency. Thus, we identified ZNF545 as a novel tumor suppressor inducing tumor cell apoptosis, repressing ribosome biogenesis and target gene transcription. The tumor-specific methylation of ZNF545 could be an epigenetic biomarker for cancer diagnosis. Mol Cancer Res; 10(7); 925-36. Ó2012 AACR.

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“…A genome-wide screen of 44 MoMuLVinduced T cell lymphomas for novel targets of proviral DNA integration yielded clones of 149 independent provirus integrations. Six of these integrations, cloned from five independent tumors, had targeted a gene we named Ndy1, also known as FBXL10 or JHDM1B (9,10,16,17). Two of them were cloned from a single tumor, D0, suggesting that this tumor consists of at least two populations of cells, both of which carry an inte-grated provirus in this locus.…”

Section: Ndy1 Is a Common Target Of Provirus Integration In Momulv-inmentioning

confidence: 99%

“…Ndy1 encodes a protein that contains a JmjC domain (9,10,16,17), a CXXC zinc finger, a PHD zinc finger, a proline-rich region (PRR), an F-box, and a leucine-rich repeat (LRR) (Fig. 1 A and ref.…”

Section: Ndy1 Is a Common Target Of Provirus Integration In Momulv-inmentioning

confidence: 99%

Members of a family of JmjC domain-containing oncoproteins immortalize embryonic fibroblasts via a JmjC domain-dependent process

Pfau

Tzatsos

Kampranis

et al. 2008

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

115

146

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A common integration site, cloned from MoMuLV-induced rat T cell lymphomas, was mapped immediately upstream of Not dead yet-1 (Ndy1)/KDM2B, a gene expressed primarily in testis, spleen, and thymus, that is also known as FBXL10 or JHDM1B. Ndy1 encodes a nuclear, chromatin-associated protein that harbors Jumonji C (JmjC), CXXC, PHD, proline-rich, F-box, and leucine-rich repeat domains. Ndy1 and its homolog Ndy2/KDM2A (FBXL11 or JHDM1A), which is also a target of provirus integration in retrovirus-induced lymphomas, encode proteins that were recently shown to possess Jumonji C-dependent histone H3 K36 dimethyldemethylase or histone H3 K4 trimethyl-demethylase activities. Here, we show that mouse embryo fibroblasts engineered to express Ndy1 or Ndy2 undergo immortalization in the absence of replicative senescence via a JmjC domain-dependent process that targets the Rb and p53 pathways. Knockdown of endogenous Ndy1 or expression of JmjC domain mutants of Ndy1 promote senescence, suggesting that Ndy1 is a physiological inhibitor of senescence in dividing cells and that inhibition of senescence depends on histone H3 demethylation.cancer ͉ histone demethylase ͉ immortalization ͉ senescence ͉ insertional mutagenesis

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JHDM1B/FBXL10 is a nucleolar protein that represses transcription of ribosomal RNA genes

Cited by 250 publications

References 30 publications

Selective recruitment of breast cancer anti-estrogen resistance genes and relevance for breast cancer progression and tamoxifen therapy response

Selective recruitment of breast cancer anti-estrogen resistance genes and relevance for breast cancer progression and tamoxifen therapy response

A Novel 19q13 Nucleolar Zinc Finger Protein Suppresses Tumor Cell Growth through Inhibiting Ribosome Biogenesis and Inducing Apoptosis but Is Frequently Silenced in Multiple Carcinomas

Members of a family of JmjC domain-containing oncoproteins immortalize embryonic fibroblasts via a JmjC domain-dependent process

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