碱性成纤维细胞生长因子需要蛋白激酶C的长期激活来诱导转化胎牛主动脉内皮细胞的细胞增殖。

M Presta, L Tiberio, M Rusnati, P Dell'Era, G Ragnotti
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引用次数: 66

摘要

碱性成纤维细胞生长因子(bFGF)诱导转化胎牛主动脉内皮GM 7373细胞的蛋白激酶C (PKC)依赖性有丝分裂反应。诱导细胞增殖需要bFGF与细胞的长期相互作用。事实上,bFGF处理的细胞只有在进入细胞周期的S期(即bFGF处理开始后12-14小时)后才会开始增殖。在此之前,对bFGF的有丝分裂反应是通过以下方式消除的:1)苏拉明去除细胞外bFGF, 2)在培养基中加入中和性抗bFGF抗体,3)蛋白激酶抑制剂H-7抑制PKC活性,4)与佛波酯共处理下调PKC活性。因此,bFGF与细胞长时间相互作用的需求反映了PKC长时间激活的需求。同样的结论也适用于PKC活化剂12- o -十四烷醇、13-乙酸酯和1,2-二辛烷醇-sn-甘油。这两种分子分别需要激活PKC 16和6小时才能诱导50%的最大细胞增殖。PKC对持久激活的要求似乎是一种控制细胞增殖的机制,能够区分短暂的非有丝分裂刺激和持久的有丝分裂刺激。
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Basic fibroblast growth factor requires a long-lasting activation of protein kinase C to induce cell proliferation in transformed fetal bovine aortic endothelial cells.

Basic fibroblast growth factor (bFGF) induces a protein kinase C (PKC)-dependent mitogenic response in transformed fetal bovine aortic endothelial GM 7373 cells. A long-lasting interaction of bFGF with the cell is required to induce cell proliferation. bFGF-treated cells are in fact committed to proliferate only after they have entered the phase S of the cell cycle, 12-14 h after the beginning of bFGF treatment. Before that time, the mitogenic response to bFGF is abolished by 1) removal of extracellular bFGF by suramin, 2) addition of neutralizing anti-bFGF antibodies to the culture medium, 3) inhibition of PKC activity by the protein kinase inhibitor H-7, and 4) down-regulation of PKC by cotreatment with phorbol ester. Thus the requirement for a prolonged interaction of bFGF with the cell reflects the requirement for a prolonged activation of PKC. Similar conclusions can be drawn for the PKC activators 12-O-tetradecanoyl phorbol 13-acetate and 1,2-dioctanoyl-sn-glycerol. The two molecules require 16 and 6 h, respectively, of activation of PKC to induce 50% of maximal cell proliferation. The requirement for a long-lasting activation of PKC appears to be a mechanism for the control of cell proliferation capable of discriminating among transient nonmitogenic stimuli and long-lasting mitogenic stimuli.

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