Farnesylated RhoB inhibits radiation-induced mitotic cell death and controls radiation-induced centrosome overduplication

Milia, Julie; Teyssier, Franck; Dalenc, Florence; Ader, Isabelle; Delmas, Caroline; Pradines, Anne; Lajoie‐Mazenc, Isabelle; Baron, Rudi; Bonnet, Jacques; Cohen–Jonathan, Elizabeth; Favre, Gilles; Toulas, Christine

doi:10.1038/sj.cdd.4401586

Cited by 35 publications

(22 citation statements)

References 33 publications

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“…Enhancement of the efficacy of 5-fluorouracil against pancreatic tumors by methionine stress is supported by the observed down-regulation of TYMS, DTYMK, and UP, which are involved in 5-fluorouracil metabolism, and FEN1, FANCG, and RAD23B, which are involved in the repair of 5-fluorouracil-induced DNA damage (45). Enhancement of the efficacy to radiation by methionine stress is supported by the observed down-regulation of RhoB expression, the farnesylated form of which inhibits radiation-induced mitotic cell death (46). Synergy between methionine stress and alkylating agents has been shown in the past (14) but has not been fully investigated.…”

Section: Discussionmentioning

confidence: 62%

Modulation of cell cycle and gene expression in pancreatic tumor cell lines by methionine deprivation (methionine stress): implications to the therapy of pancreatic adenocarcinoma

Kokkinakis

Liu

Neuner

2005

Molecular Cancer Therapeutics

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Section: Discussionmentioning

confidence: 62%

Modulation of cell cycle and gene expression in pancreatic tumor cell lines by methionine deprivation (methionine stress): implications to the therapy of pancreatic adenocarcinoma

Kokkinakis

Liu

Neuner

2005

Molecular Cancer Therapeutics

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“…Thus, RhoB-GG suppresses Ras transformation in NIH 3T3 cells while RhoB-F potentiates transformation [9]. In contrast, RhoB-F can provide resistance to radiation-induced cell death in NIH 3T3 cells while RhoB-GG does not provide such protection [34]. The precise signaling activities that mediate these differences in signaling potential have not been delineated.…”

Section: Discussionmentioning

confidence: 99%

“…In a recent study Milia et al showed that RhoB-F (but not RhoB-GG) is required to confer resistance to radiation-induced mitotic cell death in mouse embryonic fibroblasts and that this function is dependent on ROCK I [34]. In addition, ROCK I has been reported to mediate thrombininduced NF-κB activation in endothelial cells, which in part can be attributed to increased phosphorylation of the transactivation domain of RelA/p65 [35].…”

Section: Rhob Activates Nf-κb In a Rock-dependent Mannermentioning

confidence: 99%

ROCK I-mediated activation of NF-κB by RhoB

Rodrı́guez

Sahay

Olabisi

et al. 2007

Cellular Signalling

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RhoB is a short-lived protein whose expression is increased by a variety of extra-cellular stimuli including UV irradiation, epidermal growth factor (EGF) and transforming growth factor β (TGF-β). Whereas most Rho proteins are modified by the covalent attachment of a geranylgeranyl group, RhoB is unique in that it can exist in either a geranylgeranylated (RhoB-GG) or a farnesylated (RhoB-F) form. Although each form is proposed to have different cellular functions, the signaling events that underlie these differences are poorly understood. Here we show that RhoB can activate NF-κB signaling in multiple cell types. Whereas RhoB-F is a potent activator of NF-κB, much weaker activation is observed for RhoB-GG, RhoA, and RhoC. NF-κB activation by RhoB is not associated with increased nuclear translocation of RelA/p65, but rather, by modification of the RelA/p65 transactivation domain. Activation of NF-κB by RhoB is dependent upon ROCK I but not PRK I. Thus, ROCK I cooperates with RhoB to activate NF-κB, and suppression of ROCK I activity by genetic or pharmacological inhibitors blocks NF-κB activation. Suppression of RhoB activity by dominant-inhibitory mutants, or siRNA, blocks NF-κB activation by Bcr, and TSG101, but not by TNFα or oncogenic Ras. Collectively, these observations suggest the existence of an endosomeassociated pathway for NF-κB activation that is preferentially regulated by the farnesylated form of RhoB.

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“…As expected, FGFR1 was silenced in the two selected U87 clones [clones 2 and 7; FGFR1(À)U87 cells], which present a significant FGFR1 inhibition of 67.1% and 38.1%, respectively ( We then deciphered the biological pathways sustaining the radioprotective effect of FGFR1 in glioblastoma cells. Because we largely demonstrated that the radiation-induced cell death of solid tumor cells is mitotic cell death (6,11,21,22), we first determined the number of giant multinucleated cells 5 days after 8 Gy irradiation when FGFR1 has been silenced or not. As shown in Fig.…”

Section: Fgfr1 Inhibition Increases the Glioblastoma Cells Sensitivitmentioning

confidence: 99%

“…The number of centrosomes in U87 and LN18 cells was analyzed using immunofluorescence staining for g-tubulin as already described (11,22).…”

Section: Evaluation Of the Centrosomes Duplicationmentioning

confidence: 99%

FGFR1 Induces Glioblastoma Radioresistance through the PLCγ/Hif1α Pathway

et al. 2016

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FGF2 signaling in glioblastoma induces resistance to radiotherapy, so targeting FGF2/FGFR pathways might offer a rational strategy for tumor radiosensitization. To investigate this possibility, we evaluated a specific role for FGFR1 in glioblastoma radioresistance as modeled by U87 and LN18 glioblastomas in mouse xenograft models. Silencing FGFR1 decreased radioresistance in a manner associated with radiation-induced centrosome overduplication and mitotic cell death. Inhibiting PLCg (PLCG1), a downstream effector signaling molecule for FGFR1, was sufficient to produce similar effects, arguing that PLCg is an essential mediator of FGFR1-induced radioresistance. FGFR1 silencing also reduced expression of HIF1a, which in addition to its roles in hypoxic responses exerts an independent effect on radioresistance. Finally, FGFR1 silencing delayed the growth of irradiated tumor xenografts, in a manner that was associated with reduced HIF1a levels but not blood vessel alterations. Taken together, our results offer a preclinical proof of concept that FGFR1 targeting can degrade radioresistance in glioblastoma, a widespread problem in this tumor, prompting clinical investigations of the use of FGFR1 inhibitors for radiosensitization. Cancer Res; 76(10); 3036-44. Ó2016 AACR.

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Farnesylated RhoB inhibits radiation-induced mitotic cell death and controls radiation-induced centrosome overduplication

Cited by 35 publications

References 33 publications

Modulation of cell cycle and gene expression in pancreatic tumor cell lines by methionine deprivation (methionine stress): implications to the therapy of pancreatic adenocarcinoma

Modulation of cell cycle and gene expression in pancreatic tumor cell lines by methionine deprivation (methionine stress): implications to the therapy of pancreatic adenocarcinoma

ROCK I-mediated activation of NF-κB by RhoB

FGFR1 Induces Glioblastoma Radioresistance through the PLCγ/Hif1α Pathway

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