| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 9308407 | Kidney International | 2005 | 13 Pages |
Abstract
FTS (5-20 μmol/L) inhibits PDGF-induced but not serum-induced HMC proliferation. FTS (10-20 μmol/L) also promotes HMC apoptosis in the presence of PDGF but not serum. These effects appear to be mediated by inhibitory effects on Ras-dependent signaling that occur as a result of the dislodgment of Ras from its membrane-anchorage sites by FTS. The selectivity of FTS toward PDGF-driven HMC proliferation suggests that FTS may be a valuable therapeutic in mesangioproliferative renal disease.
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Authors
Arif Khwaja, Claire C. Sharpe, Mazhar Noor, Yoel Kloog, Bruce M. Hendry,