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β型转化生长因子的抗增殖作用发生在远离生长激活因子受体的水平。

The antiproliferative effect of type beta transforming growth factor occurs at a level distal from receptors for growth-activating factors.

作者信息

Like B, Massagué J

出版信息

J Biol Chem. 1986 Oct 15;261(29):13426-9.

PMID:2875996
Abstract

Transforming growth factor-beta (TGF beta) from human platelets blocks the ability of Mv1Lu mink lung epithelial cells to grow in response to serum mitogens, epidermal growth factor (EGF), or insulin. The phenotypic response of Mv1Lu cells to TGF beta is characterized by a flat, very enlarged cell morphology and a markedly increased production and accumulation of extracellular matrix fibronectin. The ability of TGF beta to alter the ligand binding or signal transducing activity of mitogen receptors in Mv1Lu cells has been examined. In contrast to NRK-49F rat fibroblasts, Mv1Lu cells do not respond to TGF beta with a decrease in the affinity or a change in the number of cell surface receptors for EGF. Soluble extracts from Mv1Lu cells contain a protein kinase activity which selectively phosphorylates ribosomal protein S6; this S6 kinase activity is elevated severalfold minutes after exposure of cells to mitogens. This kinase activity has been used as the parameter to measure the signaling ability of EGF receptors and insulin receptors in cells treated with TGF beta. We find that TGF beta does not alter the basal level of S6 kinase activity or its elevation by EGF or insulin. In TGF beta-treated cells rendered insensitive to the growth-promoting action of EGF, the parameters of elevation of S6 kinase activity by EGF are similar to those of control, growth-competent cells. The results suggest that TGF beta inhibits cell proliferation by acting at a level distal from the receptors for growth-activating factors.

摘要

人血小板中的转化生长因子-β(TGF-β)可阻断Mv1Lu貂肺上皮细胞对血清促细胞分裂剂、表皮生长因子(EGF)或胰岛素作出反应而生长的能力。Mv1Lu细胞对TGF-β的表型反应的特征是细胞形态扁平且极度增大,以及细胞外基质纤连蛋白的产生和积累显著增加。已对TGF-β改变Mv1Lu细胞中有丝分裂原受体的配体结合或信号转导活性的能力进行了研究。与NRK-49F大鼠成纤维细胞不同,Mv1Lu细胞对TGF-β的反应不是EGF细胞表面受体的亲和力降低或数量改变。Mv1Lu细胞的可溶性提取物含有一种蛋白激酶活性,该活性可选择性地使核糖体蛋白S6磷酸化;在细胞暴露于促细胞分裂剂后几分钟,这种S6激酶活性会升高几倍。这种激酶活性已被用作衡量TGF-β处理的细胞中EGF受体和胰岛素受体信号传导能力的参数。我们发现,TGF-β不会改变S6激酶活性的基础水平,也不会改变其被EGF或胰岛素升高的水平。在用TGF-β处理并对EGF的促生长作用不敏感的细胞中,EGF使S6激酶活性升高的参数与对照的、具有生长能力的细胞相似。结果表明,TGF-β通过在远离生长激活因子受体的水平起作用来抑制细胞增殖。

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