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Curr Oncol. 2009 Mar;16(2):36-43.

Development of cell-cycle inhibitors for cancer therapy.

Author information

  • 1Department of Medicine, Division of Solid Tumor Oncology, Melanoma and Sarcoma Service, Memorial Sloan-Kettering Cancer Center, New York, NY, U.S.A.

Abstract

The cell cycle governs the transition from quiescence through cell growth to proliferation. The key parts of the cell cycle machinery are the cyclin-dependent kinases (CDKS) and the regulatory proteins called cyclins. The CDKS are rational targets for cancer therapy because their expression in cancer cells is often aberrant and their inhibition can induce cell death. Inhibitors of CDKS can also block transcription.Several drugs targeting the cell cycle have entered clinical trials. These agents include flavopiridol, indisulam, AZD5438, SNS-032, bryostatin-1, seliciclib, PD 0332991, and SCH 727965. Phase i studies have demonstrated that these drugs can generally be administered safely. Phase ii studies have shown little single-agent activity in solid tumors, but combination studies with cytotoxic chemotherapy have been more promising. In hematologic malignancies, reports have shown encouraging single-agent and combination activity. Pharmacodynamic studies show that the dose and schedule of these drugs are crucial to permit maximum therapeutic effect.

KEYWORDS:

Cell cycle; cyclin-dependent kinases; cyclins; phase i clinical trials; phase ii clinical trials

PMID:
19370178
[PubMed]
PMCID:
PMC2669234
Free PMC Article
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