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转化生长因子-β诱导人骨癌细胞的有丝分裂增殖。

Transforming growth factor-beta-induced mitogenesis of human bone cancer cells.

作者信息

Datta H K, Zaidi M, Champaneri J B, MacIntyre I

机构信息

Department of Chemical Pathology, Royal Postgraduate Medical School, London, United Kingdom.

出版信息

Biochem Biophys Res Commun. 1989 Jun 15;161(2):672-6. doi: 10.1016/0006-291x(89)92651-x.

Abstract

We report for the first time the bifunctional effects of transforming growth factor-beta on the growth of cloned human osteosarcoma cells (Htb96). Cell growth was assessed by determining the cell number, replication index and [3H]-thymidine incorporation following 48 hours incubation of cultured Htb96 cells with the peptide. Exposure of cells to concentrations of TGF-beta upto 40 pM caused a mitogenic response, concentrations between 40 and 800 pM failed to stimulate cell growth and higher doses caused an inhibition of cell proliferation. The initial cell density was found to alter the responsiveness of Htb96 cells to TGF-beta; stimulation of proliferation was less profound at high and low cell densities. The observed cell density- and growth factor concentration-dependent effects of TGF-beta on the growth of tumour cells might suggest the existence of an autocrine regulatory mechanism. Furthermore, by demonstrating a sensitivity to inhibition by indomethacin, we conclude that the proliferative effect of TGF-beta is at least, in part, dependent on the de novo synthesis of prostaglandins.

摘要

我们首次报道了转化生长因子-β对克隆的人骨肉瘤细胞(Htb96)生长的双功能作用。通过在培养的Htb96细胞与该肽孵育48小时后测定细胞数量、复制指数和[3H] - 胸苷掺入量来评估细胞生长。将细胞暴露于高达40 pM浓度的转化生长因子-β会引起促有丝分裂反应,40至800 pM之间的浓度未能刺激细胞生长,而更高剂量则会抑制细胞增殖。发现初始细胞密度会改变Htb96细胞对转化生长因子-β的反应性;在高细胞密度和低细胞密度下,增殖刺激作用不那么显著。观察到的转化生长因子-β对肿瘤细胞生长的细胞密度和生长因子浓度依赖性效应可能表明存在自分泌调节机制。此外,通过证明对吲哚美辛抑制的敏感性,我们得出结论,转化生长因子-β的增殖作用至少部分取决于前列腺素的从头合成。

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