Differences of Cell Growth and Cell Cycle Regulators Induced by Basic Fibroblast Growth Factor Between Nifedipine Responders and Non-responders

Differences of cell proliferation, cell cycle, and G1/S transition regulatory proteins of gingival fibroblasts derived from nifedipine-reactive patient (NIFr) and nifedipine-non-reactive patient (NIFn) in the presence of basic fibroblast growth factor (bFGF) were investigated to elucidate the mechan...

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Main Authors: Reiri Takeuchi (Author), Hiroko Matsumoto (Author), Hidehiko Okada (Author), Mami Hori (Author), Akihiko Gunji (Author), Kosuke Hakozaki (Author), Yoshiaki Akimoto (Author), Akira Fujii (Author)
Format: Book
Published: Elsevier, 2007-01-01T00:00:00Z.
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Summary:Differences of cell proliferation, cell cycle, and G1/S transition regulatory proteins of gingival fibroblasts derived from nifedipine-reactive patient (NIFr) and nifedipine-non-reactive patient (NIFn) in the presence of basic fibroblast growth factor (bFGF) were investigated to elucidate the mechanism of gingival overgrowth associated with nifedipine, one of the Ca2+-channel blockers. The proliferation rate of NIFr cells in the presence of bFGF significantly increased than NIFn cells. The proportion of NIFr cells that had undergone progression to the S and G2/M phases from the G0/G1 phase significantly increased compared to that in NIFn cells. Increases of pRB (Ser807/811), pCDK2 (Thr160), CDK2, and cyclin E protein levels in NIFr cells were greater than those in NIFn cells. The elevations of pRB (Ser780), RB, and cyclin A protein levels in NIFr cells did not differ from those of NIFn cells. The growth of NIFr cells was greater than that of NIFn cells as a result of the active G1/S transition of NIFr cells, as assessed by the increments of cyclin E, pCDK2, and pRB (ser807/811) protein in NIFr cells. Keywords:: gingival overgrowth, nifedipine, gingival fibroblast, cell cycle
Item Description:1347-8613
10.1254/jphs.FP0060928