In vitro activity of cyclin-dependent kinase inhibitor CYC202 (Seliciclib, R-roscovitine) in mantle cell lymphomas

doi:10.1093/annonc/mdi217

Annals of Oncology Advance Access originally published online on April 25, 2005
Annals of Oncology 2005 16(7):1169-1176; doi:10.1093/annonc/mdi217

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In vitro activity of cyclin-dependent kinase inhibitor CYC202 (Seliciclib, R-roscovitine) in mantle cell lymphomas

K. Lacrima¹, A. Valentini¹, C. Lambertini¹, M. Taborelli¹, A. Rinaldi¹, E. Zucca², C. Catapano¹, F. Cavalli¹^,2, A. Gianella-Borradori³, D. E. MacCallum³ and F. Bertoni¹^,4^,*

¹ Experimental Oncology and ² Lymphoma Unit, Oncology Institute of Southern Switzerland, Bellinzona, Switzerland; ³ Cyclacel Ltd, Dundee, Scotland, UK; ⁴ Experimental Haematology, St Bartholomew's Hospital and The London Hospital, London, UK

*Correspondence to:Dr F. Bertoni, Experimental Oncology, Oncology Institute of Southern Switzerland, via Vincenzo Vela 6, 6500 Bellinzona, Switzerland. Tel: +41 (0)91 8200 367; Fax: +41 (0)91 8200 397; Email: frbertoni{at}mac.com

Background:: Mantle cell lymphoma (MCL) has the worst prognosisof all B-cell lymphomas and has poor response to conventionaltherapy. It is characterized by the presence of a chromosomaltranslocation t(11:14) (q13;q32) which results in deregulatedcyclin D₁ expression. Since defects in cell cycle regulationand apoptosis are primary events in MCL, small-molecule inhibitorsof cdks–cyclins may play an important role in the therapyof this disorder. CYC202 (Seliciclib, R-roscovitine; CyclacelLtd., Dundee, UK) is a purine analogue and a selective inhibitorof the cdk2–cyclin E as well as cdk7–cyclin H andcdk9–cyclin T.

Materials and methods:: The activity of CYC202 was tested infour human MCL cell lines: REC, Granta-519, JeKo-1 and NCEB-1.The effect of CYC202 on the cell cycle and on apoptosis-, cell-cycle-and transcription-regulation-related proteins was assessed.

Results:: The IC₅₀ was 25 µM for REC, Granta-519 and JeKo-1cells and 50 µM for NCEB-1 cells. CYC202 caused an accumulationof cells in the G₂–M phase of the cell cycle and apoptosis.CYC202 caused down-regulation of cyclin D₁ and Mcl-1 proteinlevels, possibly because of the inhibition of transcriptionelongation.

Conclusions:: Our data suggest that CYC202 is an active agentin MCL. The concomitant decrease of the phosphorylated and totalforms of RNA polymerase II suggests that this could be the mainmechanism mediating the biological effects of CYC202 in MCLcells. The drug might represent a new therapeutic agent in thislymphoma subtype.

Key words: apoptosis, cdk inhibitor, cyclin D1, lymphoma

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