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INVOLVEMENT OF BASIC FIBROBLAST GROWTH-FACTOR IN SURAMIN-INDUCED INHIBITION OF V79/AP4 FIBROBLAST CELL-PROLIFERATION

机译:碱性成纤维细胞生长因子参与苏拉明诱导的V79 / AP4成纤维细胞增殖的抑制

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摘要

The V79/AP4 Chinese hamster fibroblasts were densely stained with the anti-basic fibroblast growth factor (bFGF) antibody demonstrating an endogenous production of the peptide. The in vitro proliferation of these cells was stimulated by exogenous bFGF and the maximum growth (259% increase in H-3-thymidine incorporation into DNA) was reached with bFGF 10 ng ml-1. Inhibition of bFGF-mediated mitogenic pathway was obtained with a 15-mer antisense oligodeoxynucleotide targeted against bFGF mRNA and with suramin, a drug which blocks the biological activity of heparin-binding growth factors. bFGF antisense oligomer reduced the synthesis of DNA by 79.5 and 89.5% at 20 and 60 muM, respectively; this effect was reversed by the addition of exogenous bFGF to the culture medium. A short-term exposure to suramin 300 mug ml-1 produced a modest reduction in H-3-thymidine incorporation but suppressed the mitogenic effect of bFGF on V79/AP4 cells. In cells treated with suramin 300 mug ml-1 the drug concentration increased linearly over 3 days, reaching 13.15 mug mg-1 of protein; cell proliferation was inhibited in a dose-related manner as evaluated by the colony formation assay (IC50: 344.22 mug ml-1) and by the number of mitoses observed in culture. Furthermore, the drug induced ultrastructural alterations, consisting of perinuclear cisternae swelling, chromatin condensation, nucleolar segregation and cytoplasmic vacuolations. These findings demonstrated that the endogenous production of bFGF plays an important role in V79/AP4 fibroblasts proliferation, and the inhibition of bFGF-mediated mitogenic signalling with bFGF antisense oligomer or suramin is an effective mean of reducing cell growth.
机译:V79 / AP4中国仓鼠成纤维细胞用抗碱性成纤维细胞生长因子(bFGF)抗体密集染色,证明了该肽的内源性产生。这些细胞的体外增殖受到外源性bFGF的刺激,而bFGF 10 ng ml-1达到了最大的生长(H-3-胸苷掺入DNA的增加259%)。用针对bFGF mRNA的15-mer反义寡脱氧核苷酸和苏拉明(一种阻止肝素结合生长因子的生物学活性的药物)获得了bFGF介导的促有丝分裂途径的抑制作用。 bFGF反义寡聚物在20和60μM时分别使DNA的合成减少了79.5和89.5%。通过向培养基中添加外源性bFGF,可以逆转这种效应。短期暴露于苏拉明300杯ml-1中可适度减少H-3-胸苷的掺入,但可抑制bFGF对V79 / AP4细胞的促有丝分裂作用。在用苏拉明300杯ml-1处理的细胞中,药物浓度在3天内线性增加,达到13.15杯mg-1的蛋白质。通过菌落形成试验(IC50:344.22马克杯ml-1)和在培养物中观察到的有丝分裂的数量来评估,细胞增殖以剂量相关的方式被抑制。此外,该药物诱导超微结构改变,包括核周池肿胀,染色质浓缩,核仁分离和细胞质空泡化。这些发现表明,bFGF的内源性产生在V79 / AP4成纤维细胞增殖中起重要作用,而bFGF反义寡聚物或苏拉明对bFGF介导的有丝分裂信号的抑制是减少细胞生长的有效手段。

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