P276-00, a cyclin-dependent kinase inhibitor, modulates cell cycle and induces apoptosis in vitro and in vivo in mantle cell lymphoma cell lines.

Abstract	BACKGROUND: Mantle cell lymphoma (MCL) is a well-defined aggressive lymphoid neoplasm characterized by proliferation of mature B-lymphocytes that have a remarkable tendency to disseminate. This tumor is considered as one of the most aggressive lymphoid neoplasms with poor responses to conventional chemotherapy and relatively short survival. Since cyclin D1 and cell cycle control appears as a natural target, small-molecule inhibitors of cyclin-dependent kinases (Cdks) and cyclins may play important role in the therapy of this disorder. We explored P276-00, a novel selective potent Cdk4-D1, Cdk1-B and Cdk9-T1 inhibitor discovered by us against MCL and elucidated its potential mechanism of action. METHODS: The cytotoxic effect of P276-00 in three human MCL cell lines was evaluated in vitro. The effect of P276-00 on the regulation of cell cycle, apoptosis and transcription was assessed, which are implied in the pathogenesis of MCL. Flow cytometry, western blot, immunoflourescence and siRNA studies were performed. The in vivo efficacy and effect on survival of P276-00 was evaluated in a Jeko-1 xenograft model developed in SCID mice. PK/PD analysis of tumors were performed using LC-MS and western blot analysis. RESULTS: P276-00 showed a potent cytotoxic effect against MCL cell lines. Mechanistic studies confirmed down regulation of cell cycle regulatory proteins with apoptosis. P276-00 causes time and dose dependent increase in the sub G1 population as early as from 24 h. Reverse transcription PCR studies provide evidence that P276-00 treatment down regulated transcription of antiapoptotic protein Mcl-1 which is a potential pathogenic protein for MCL. Most importantly, in vivo studies have revealed significant efficacy as a single agent with increased survival period compared to vehicle treated. Further, preliminary combination studies of P276-00 with doxorubicin and bortezomib showed in vitro synergism. CONCLUSION: Our studies thus provide evidence and rational that P276-00 alone or in combination is a potential therapeutic molecule to improve patients' outcome in mantle cell lymphoma.
Authors	Nitesh P Shirsath, Sonal M Manohar, Kalpana S Joshi
Journal	Molecular cancer (Mol Cancer) Vol. 11 Pg. 77 (Oct 18 2012) ISSN: 1476-4598 [Electronic] England
PMID	23075291 (Publication Type: Journal Article, Research Support, Non-U.S. Gov't)
Chemical References	Antigens, Surface Antineoplastic Agents Boronic Acids CCND1 protein, human Flavones LY86 protein, human Neoplasm Proteins P276-00 Protein Kinase Inhibitors Pyrazines RNA, Small Interfering Cyclin D1 Bortezomib Doxorubicin
Topics	Animals Antigens, Surface (genetics, metabolism) Antineoplastic Agents (pharmacology) Apoptosis (drug effects) Boronic Acids (pharmacology) Bortezomib Cell Cycle (drug effects) Cell Line, Tumor Cyclin D1 (genetics, metabolism) Dose-Response Relationship, Drug Doxorubicin (pharmacology) Drug Synergism Flavones (pharmacology) Gene Expression Regulation, Neoplastic (drug effects) Humans Inhibitory Concentration 50 Lymphoma, Mantle-Cell (drug therapy, enzymology, pathology) Mice Mice, SCID Neoplasm Proteins (genetics, metabolism) Protein Kinase Inhibitors (pharmacology) Pyrazines (pharmacology) RNA, Small Interfering (genetics, metabolism) Survival Analysis Xenograft Model Antitumor Assays

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