Identification of kinetin riboside as a repressor of CCND1 and CCND2 with preclinical antimyeloma activity
Rodger E. Tiedemann, Xinliang Mao, Chang-Xin Shi, Yuan Xiao Zhu, Stephen E. Palmer, Michael Sebag, Ron Marler, Marta Chesi, Rafael Fonseca, P. Leif Bergsagel, Aaron D. Schimmer, A. Keith Stewart
Rodger E. Tiedemann, Xinliang Mao, Chang-Xin Shi, Yuan Xiao Zhu, Stephen E. Palmer, Michael Sebag, Ron Marler, Marta Chesi, Rafael Fonseca, P. Leif Bergsagel, Aaron D. Schimmer, A. Keith Stewart
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Research Article Oncology

Identification of kinetin riboside as a repressor of CCND1 and CCND2 with preclinical antimyeloma activity

Abstract

Knockout and transgenic studies in mice demonstrate that normal somatic tissues redundantly express 3 cyclin D proteins, whereas tumor cells seem dependent on a single overexpressed cyclin D. Thus, selective suppression of the individual cyclin D deregulated in a tumor represents a biologically valid approach to targeted cancer therapy. In multiple myeloma, overexpression of 1 of the cyclin D proteins is a ubiquitous feature, unifying at least 7 different initiating genetic events. We demonstrate here that RNAi of genes encoding cyclin D1 and cyclin D2 (CCND1 and CCND2, respectively) inhibits proliferation and is progressively cytotoxic in human myeloma cells. By screening a chemical library using a cell-based assay for inhibition of CCND2 trans-activation, we identified the plant cytokinin kinetin riboside as an inhibitor of CCND2 trans-activation. Kinetin riboside induced marked suppression of CCND2 transcription and rapidly suppressed cyclin D1 and D2 protein expression in primary myeloma cells and tumor lines, causing cell-cycle arrest, tumor cell–selective apoptosis, and inhibition of myeloma growth in xenografted mice. Mechanistically, kinetin riboside upregulated expression of transcription repressor isoforms of cAMP-response element modulator (CREM) and blocked both trans-activation of CCND2 by various myeloma oncogenes and cis-activation of translocated CCND1, suggesting induction of an overriding repressor activity that blocks multiple oncogenic pathways targeting cyclin D genes. These data support targeted repression of cyclin D genes as a therapeutic strategy for human malignancies.

Authors

Rodger E. Tiedemann, Xinliang Mao, Chang-Xin Shi, Yuan Xiao Zhu, Stephen E. Palmer, Michael Sebag, Ron Marler, Marta Chesi, Rafael Fonseca, P. Leif Bergsagel, Aaron D. Schimmer, A. Keith Stewart

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Figure 9

Kinetin riboside induces tumor growth arrest in MY5 and 8226 myeloma tumor xenografts.

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Kinetin riboside induces tumor growth arrest in MY5 and 8226 myeloma tum...
(A) Matched pairs of nude mice bearing MY5 tumors were treated i.p. with vehicle control (open squares) or with kinetin riboside (filled squares) at a dose density escalating from 100 mg/kg once daily to 85 mg/kg 5×/daily, administered 5 days per week, commencing after mean tumor volume reached 135 mm3. Mean tumor volumes ± SEM are shown from the time of xenograft initiation (n = 4/group). (B) Nude mice bearing 8226 tumors were treated with vehicle (open squares) or with kinetin riboside (filled squares) (n = 4/group) commencing at 85 mg/kg 4 times daily (i.p. and s.c.) when the mean tumor volume exceeded 135 mm3. P value was calculated by paired t test.