| Literature DB >> 11120601 |
H R Ashar1, L James, K Gray, D Carr, M McGuirk, E Maxwell, S Black, L Armstrong, R J Doll, A G Taveras, W R Bishop, P Kirschmeier.
Abstract
SCH 66336 is a potent farnesyl transferase inhibitor (FTI) in clinical development. It efficiently prevents the membrane association of H-ras, but not K- or N-ras. Yet, in soft agar, it reverts the anchorage-independent growth of human tumor cell lines (hTCLs) harboring H-ras, K-ras, and N-ras mutations, implying that blocking farnesylation of proteins besides ras may be responsible for this effect. Experiments show that SCH 66336 altered the cell cycle distribution of sensitive human tumor cells in two distinct ways. Most sensitive hTCLs accumulated in the G(2)-->M phase after the FTI treatment, but those with an activated H-ras accumulated in G(1) phase, suggesting that the biological effects induced by FTIs in cells with an activated H-ras are distinct from other sensitive cells. A careful genotypic comparison of the hTCLs revealed that those cells with wild-type p53 are especially sensitive to the FTIs. In these cells p53 and its downstream target gene p21(Cip1) are induced after treatment with SCH 66336 for 24 h. These data suggest that cell cycle effects, either G(1) or G(2)-->M accumulation, and p53 status are important for mediating the effects of FTIs on tumor cells. Copyright 2001 Academic Press.Entities:
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Year: 2001 PMID: 11120601 DOI: 10.1006/excr.2000.5076
Source DB: PubMed Journal: Exp Cell Res ISSN: 0014-4827 Impact factor: 3.905