A phase I trial of the selective oral cyclin-dependent kinase inhibitor seliciclib (CYC202; R-Roscovitine), administered twice daily for 7 days every 21 days

Benson, Charlotte; White, Jeff; Bono, Johann S. de; O’Donnell, Anne E.; Raynaud, Florence I.; Cruickshank, Clare; McGrath, Helen E.; Walton, Mike I.; Workman, Paul; Kaye, Stan B.; Cassidy, James T.; Gianella‐Borradori, Athos; Judson, Ian; Twelves, Chris

doi:10.1038/sj.bjc.6603509

Cited by 235 publications

(181 citation statements)

References 28 publications

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“…cases, in combination with nongenotoxic agents. 30 A model based on our study is presented in Figure 8. In this study, we have shown that R-Roscovitine inhibits TNFa-induced NF-kB pathway through inhibition of the IKK kinase activity and phosphorylation and degradation of IkBa.…”

Section: R-roscovitine Inhibitsmentioning

confidence: 99%

R-Roscovitine simultaneously targets both the p53 and NF-κB pathways and causes potentiation of apoptosis: implications in cancer therapy

Dey

Wong²,

Cheok

et al. 2007

Cell Death Differ

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Seliciclib (CYC202, R-Roscovitine) is a 2, 6, 9-substituted purine analog that is currently in phase II clinical trials as an anticancer agent. We show in this study that R-Roscovitine can downregulate nuclear factor-kappa B (NF-jB) activation in response to tumor necrosis factor (TNF)a and interleukin 1. Activation of p53-dependent transcription is not compromised when RRoscovitine is combined with TNFa. We characterize the molecular mechanism governing NF-jB repression and show that RRoscovitine inhibits the IjB kinase (IKK) kinase activity, which leads to defective IjBa phosphorylation, degradation and hence nuclear function of NF-jB. We further show that the downregulation of the NF-jB pathway is also at the level of p65 modification and that the phosphorylation of p65 at Ser 536 is repressed by R-Roscovitine. Consistent with repression of canonical IKK signaling pathway, the induction of NF-jB target genes monocyte chemoattractant protein, intercellular adhesion molecule-1, cyclooxygenase-2 and IL-8 is also inhibited by R-Roscovitine. We further show that treatment of cells with TNFa and RRoscovitine causes potentiation of cell death. Based on these results, we suggest the potential use of R-Roscovitine as a bitargeted anticancer drug that functions by simultaneously causing p53 activation and NF-jB suppression. This study also provides mechanistic insight into the molecular mechanism of action of R-Roscovitine, thereby possibly explaining its antiinflammatory properties. The p53 and nuclear factor-kappa B (NF-kB) pathways are two critical transcriptional regulatory networks deregulated in various human ailments including cancer and there has been a lot of evidence of cross-talk between these two pathways. 1 Activation of p53 is associated with cell cycle arrest and apoptosis while NF-kB activation is associated with cell survival. Hence, the cross-talk between these pathways must be finely tuned and regulated.p53 is one of the most extensively studied tumor suppressor proteins. 2 Loss or mutation of p53 function is correlated with increased cancer susceptibility. Hence, activating p53 has been a goal of several small molecule inhibitors currently being evaluated in the clinic.NF-kB is a transcription factor critical for the control of inflammation, apoptosis and cell proliferation. 3,4 Chronic inflammation by constitutively active NF-kB has been shown to contribute to the development of many cancers. 5 It is becoming apparent that deregulated activity of NF-kB is observed and causally linked to the development of several diseases that have an inflammatory component. 6,7 Hence, identification of NF-kB inhibitors has been the focus of several academic and pharmaceutical establishments. 6,7 Since p53 promotes cell death and NF-kB prevents cell death, an anticancer agent that simultaneously activates p53 and inhibits NF-kB would offer greater potential to target two cancer targets positively.One of the ways in which the p53 pathway has been successfully targeted is by using cyclin-dependent kinase (CDK) inhibi...

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Section: R-roscovitine Inhibitsmentioning

confidence: 99%

R-Roscovitine simultaneously targets both the p53 and NF-κB pathways and causes potentiation of apoptosis: implications in cancer therapy

Dey

Wong²,

Cheok

et al. 2007

Cell Death Differ

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“…The absence of myelosuppression, reported in preclinical and clinical studies of roscovitine [134,137], is clinically beneficial. However, low hematotoxicity of roscovitine might in reality reflect poor distribution of roscovitine to the bone marrow.…”

Section: 5mentioning

confidence: 99%

“…Alzheimer's disease, viral infections, protozoal infections, and inflammatory diseases, are ongoing. The poor pharmacokinetic profile (rapid metabolism and short elimination half-life in rodents and man) and the insufficient exposure to the drug in cancer patients may explain the modest success in clinical trials [124,131,[135][136][137]. Several attempts to overcome pharmacokinetic barriers that limit the clinical use of roscovitine are ongoing.…”

Section: 5mentioning

confidence: 99%

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From Roscovitine to CYC202 to Seliciclib – from bench to bedside: discovery and development

Zhelev

Trifonov²,

Wang³

et al. 2013

Biodiscovery

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This monograph reviews the discovery and development of the cyclindependent kinase inhibitor roscovitine (R-roscovitine, CYC202, Seliciclib). The authors summarise the in vitro and in vivo data that have formed the basis for clinical investigation of Seliciclib as an anti-cancer drug. Kinase selectivity, cellular effects and the pharmacological properties of the drug are discussed in addition to the clinical results of Seliciclib being reviewed. Novel results on the effect of the drug in cardiac hypertrophy are summarized and potential applications of Seliciclib in other therapeutic areas, including, inflammation, virology, glomerulonephritis and polycystic kidney disease, are discussed. Finally the authors argue that optimisation of the therapeutic effect of kinase inhibitors such as Seliciclib can be enhanced using a systems biology approach involving mathematical modelling of the molecular pathways regulating cell growth and division. Seliciclib -discovery and developmentBioDiscovery 2 December 2013 | Issue 10 | 1

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“…Combination studies currently recruiting patients are initiated for P276-00 administered along with radiation in head and neck squamous cell carcinoma patients, and in combination with gemcitabine in patients with advanced pancreatic cancer. A phase I clinical trial of R-roscovitine has been performed in 22 patients with advanced cancer utilizing several schedules resulting in only minor therapeutical success with hypokalemia, rash and fatigue as dose limiting side-effects (Benson et al, 2007). Further evaluation of R-roscovitine in patients with non-small cell lung cancer was described: Rroscovitine in combination with cisplatin and gemcitabine in phase I showed similar adverse events, e. g., hypokalemia, liver -glutamyltranspeptidase elevation, vomiting, and a 42.9% response rate in 14 patients (Siegel-Lakhai et al, 2005).…”

Section: Cdk Inhibitors For Cancer Therapymentioning

confidence: 99%

Cyclin-Dependent Kinases (Cdk) as Targets for Cancer Therapy and Imaging

Graf¹,

Wuest²,

Pietzsch³

2011

Advances in Cancer Therapy

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A phase I trial of the selective oral cyclin-dependent kinase inhibitor seliciclib (CYC202; R-Roscovitine), administered twice daily for 7 days every 21 days

Cited by 235 publications

References 28 publications

R-Roscovitine simultaneously targets both the p53 and NF-κB pathways and causes potentiation of apoptosis: implications in cancer therapy

R-Roscovitine simultaneously targets both the p53 and NF-κB pathways and causes potentiation of apoptosis: implications in cancer therapy

From Roscovitine to CYC202 to Seliciclib – from bench to bedside: discovery and development

Cyclin-Dependent Kinases (Cdk) as Targets for Cancer Therapy and Imaging

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