Regulation of Replicative and Stress-Induced Senescence by RSK4, which is Down-regulated in Human Tumors

López-Vicente, Laura; Armengol, Gemma; Pons, Berta; Coch, Laura; Argelaguet, Elisabet; Lleonart, Matilde E.; Hernández‐Losa, Javier; Torres, Inés de; Cajal, Santiago Ramón y

doi:10.1158/1078-0432.ccr-08-3159

Cited by 37 publications

(46 citation statements)

References 40 publications

(49 reference statements)

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“…Very few studies have reported increased tumor-derived RSK expression. Rather, accumulating evidence support the idea that at least some RSK isoforms are downregulated in certain cancers (in particular RSK3 and RSK4 [44, 45]). While our data indicate a requirement for RSK1 and RSK2 (with RSK2 playing a more important role) in Ser1134 and Ser1161 phosphorylation of SOS1 in response to growth factor stimulation, further investigation will be necessary to determine the extent RSK3 or RSK4 participate in the regulation of SOS1 in other cellular contexts.…”

Section: Discussionmentioning

confidence: 99%

RSK phosphorylates SOS1 creating 14-3-3-docking sites and negatively regulating MAPK activation

Saha

Carrière

Cheerathodi

et al. 2012

Biochemical Journal

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The extent and duration of MAPK (mitogen-activated protein kinase) signalling govern a diversity of normal and aberrant cellular outcomes. Genetic and pharmacological disruption of the MAPK-activated kinase RSK (ribosomal S6 kinase) leads to elevated MAPK activity indicative of a RSK-dependent negative feedback loop. Using biochemical, pharmacological and quantitative MS approaches we show that RSK phosphorylates the Ras activator SOS1 (Son of Sevenless homologue 1) in cultured cells on two C-terminal residues, Ser1134 and Ser1161. Furthermore, we find that RSK-dependent SOS1 phosphorylation creates 14-3-3-binding sites. We show that mutating Ser1134 and Ser1161 disrupts 14-3-3 binding and modestly increases and extends MAPK activation. Together these data suggest that one mechanism whereby RSK negatively regulates MAPK activation is via site-specific SOS1 phosphorylation.

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Section: Discussionmentioning

confidence: 99%

RSK phosphorylates SOS1 creating 14-3-3-docking sites and negatively regulating MAPK activation

Saha

Carrière

Cheerathodi

et al. 2012

Biochemical Journal

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“…RSKs are directly regulated by ERK signaling and are implicated in cell growth, survival, motility, and senescence (25)(26)(27)(28). Here, we present evidence that overexpression of RSK3 and RSK4 supports cellular proliferation under PI3K pathway blockade by inhibiting apoptosis and regulating cellular translation through phosphorylation of ribosomal proteins S6 and eIF4B.…”

Section: Introductionmentioning

confidence: 68%

RSK3/4 mediate resistance to PI3K pathway inhibitors in breast cancer

Serra¹,

Eichhorn²,

García-García³

et al. 2013

J. Clin. Invest.

112

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The PI3K signaling pathway regulates diverse cellular processes, including proliferation, survival, and metabolism, and is aberrantly activated in human cancer. As such, numerous compounds targeting the PI3K pathway are currently being clinically evaluated for the treatment of cancer, and several have shown some early indications of efficacy in breast cancer. However, resistance against these agents, both de novo and acquired, may ultimately limit the efficacy of these compounds. Here, we have taken a systematic functional approach to uncovering potential mechanisms of resistance to PI3K inhibitors and have identified several genes whose expression promotes survival under conditions of PI3K/mammalian target of rapamycin (PI3K/mTOR) blockade, including the ribosomal S6 kinases RPS6KA2 (RSK3) and RPS6KA6 (RSK4). We demonstrate that overexpression of RSK3 or RSK4 supports proliferation upon PI3K inhibition both in vitro and in vivo, in part through the attenuation of the apoptotic response and upregulation of protein translation. Notably, the addition of MEK-or RSK-specific inhibitors can overcome these resistance phenotypes, both in breast cancer cell lines and patient-derived xenograft models with elevated levels of RSK activity. These observations provide a strong rationale for the combined use of RSK and PI3K pathway inhibitors to elicit favorable responses in breast cancer patients with activated RSK.

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“…RSK4 is an outlier and functionally distinct, showing low expression compared with other RSKs, and overexpression of RSK4 may restrict cell growth (12). Several studies have reported that high expression of RSK4 in breast cancer cells is anti-oncogenic, anti-invasive, and anti-metastatic (13), and RSK4 also exhibits a tumor suppressor effect in colon and renal carcinomas (14).…”

Section: Introductionmentioning

confidence: 99%

RSK4 knockdown promotes proliferation, migration and metastasis of human breast adenocarcinoma cells

Zhu

Liu

et al. 2015

Oncology Reports

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Abstract. RSK4 has been shown to inhibit the growth of certain cancer cells. The aim of this study was to construct a lentiviral vector of RSK4-shRNA (Lenti-RSK4-shRNA) to specifically block the expression of RSK4 in the human breast adenocarcinoma cell line MCF-7, and investigate the effect of the RSK4 gene on cell proliferation and invasion in vitro and in vivo. Lenti-RSK4-shRNA was stably transfected into MCF-7 cells. RSK4 mRNA and protein expression were measured by fluorescence quantitative RT-PCR and western blot analysis. Cell proliferation was evaluated by MTT assays and flow cytometric analysis. Invasion was evaluated by Transwell assays and xenograft nude mouse models. The expression of RSK4 mRNA, Ki-67 mRNA, cyclin D1 mRNA, CXCR4 mRNA and E-cadherin mRNA of tumor xenografts were detected by fluorescence quantitative RT-PCR. Significant decreases in RSK4 mRNA and protein expression was detected in MCF-7 cells carrying lentiviral RSK4-shRNA vector. The cell proliferation was significantly promoted in the RSK4-shRNA group as compared to that in the negative and blank control group. In addition, the number of cells in the S phase in the RSK4-shRNA group was significantly greater than the blank and negative control groups (P<0.05). Furthermore, the number of invading cells was increased in the RSK4-shRNA (P<0.05). In vivo, we also found that the knockdown of RSK4 promoted tumorigenicity and migration in the xenograft nude mouse model. In addition, we showed that the RSK4 mRNA and E-cadherin mRNA expression were significantly lower in the RSK4-shRNA group compared to that in negative and blank control group (both P<0.05), while the Ki-67 mRNA, cyclin D1 mRNA and CXCR4 mRNA were higher in the shRNA group compared to that in negative and blank control group (both P<0.05). In conclusion, downregulation of RSK4 expression is indicated to be associated with tumor cell proliferation and invasion, and silencing of the RSK4 may be involved in the development and progression of breast cancer through the changes of Ki-67, cyclin D1, CXCR4 and E-cadherin, and suggesting that RSK4 may act as a potential cancer suppressor gene and therapeutic target for the treatment of breast cancer.

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Regulation of Replicative and Stress-Induced Senescence by RSK4, which is Down-regulated in Human Tumors

Cited by 37 publications

References 40 publications

RSK phosphorylates SOS1 creating 14-3-3-docking sites and negatively regulating MAPK activation

RSK phosphorylates SOS1 creating 14-3-3-docking sites and negatively regulating MAPK activation

RSK3/4 mediate resistance to PI3K pathway inhibitors in breast cancer

RSK4 knockdown promotes proliferation, migration and metastasis of human breast adenocarcinoma cells

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