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表皮生长因子:人成纤维细胞中的受体以及霍乱毒素对其作用的调节

Epidermal growth factor: receptors in human fibroblasts and modulation of action by cholera toxin.

作者信息

Hollenberg M D, Cuatrecasas P

出版信息

Proc Natl Acad Sci U S A. 1973 Oct;70(10):2964-8. doi: 10.1073/pnas.70.10.2964.

Abstract

Epidermal growth factor (EGF) stimulates both DNA and RNA synthesis in contact-inhibited human fibroblasts. Stimulation of DNA synthesis is observed at concentrations as low as 3 pM, is half-maximal at 70 pM, and is maximal at 300 pM EGF. The action of EGF is similar to that of fetal-calf serum, but is distinguished by the time-course of stimulation and by the ability of serum to stimulate further those cells maximally stimulated by EGF. Cells that synthesize DNA in response to physiological concentrations of EGF (10(-11) to 10(-10) M) are insensitive to physiological concentrations of insulin (10(-11) to 10(-10) M) and respond only minimally to very high concentrations of this hormone (10(-6) M). The biological activity of EGF is paralleled by binding of this peptide to fibroblasts in a specific and saturable manner; the dissociation constant is about 800 pM. The binding of EGF is unaffected by either insulin or cholera toxin. Cholera toxin inhibits the action of both EGF and serum. Suppression of DNA synthesis is observed at 0.02 pM toxin, and is maximal at about 2 pM. Cells treated with cholera toxin at these concentrations appear to be otherwise viable by several criteria. The stimulatory effects of EGF are also inhibited by theophylline and dibutyryl cyclic AMP separately or in combination. These observations indicate that fibroblasts possess receptors for EGF by biological and physicochemical criteria, and suggest that a similar if not identical peptide may be amongst those factors in sera which stimulate cell growth. The possibility is considered that EGF and cholera toxin modulate the ability of a cell to initiate polynucleotide synthesis by way of specific cell-surface interactions which in turn alter the levels of intracellular cyclic AMP.

摘要

表皮生长因子(EGF)可刺激接触抑制的人成纤维细胞中的DNA和RNA合成。在低至3 pM的浓度下即可观察到对DNA合成的刺激作用,在70 pM时达到最大刺激作用的一半,在300 pM EGF时达到最大刺激作用。EGF的作用与胎牛血清相似,但在刺激的时间进程以及血清对那些被EGF最大程度刺激的细胞进一步刺激的能力方面有所不同。响应生理浓度EGF(10⁻¹¹至10⁻¹⁰ M)而合成DNA的细胞对生理浓度的胰岛素(10⁻¹¹至10⁻¹⁰ M)不敏感,并且仅对这种激素的非常高浓度(10⁻⁶ M)有最小的反应。EGF的生物学活性与其以特异性和可饱和方式与成纤维细胞结合平行;解离常数约为800 pM。EGF的结合不受胰岛素或霍乱毒素的影响。霍乱毒素抑制EGF和血清的作用。在0.02 pM毒素时观察到DNA合成受到抑制,在约2 pM时达到最大抑制。通过几个标准来看,在这些浓度下用霍乱毒素处理的细胞在其他方面似乎是有活力的。茶碱和二丁酰环磷酸腺苷单独或联合使用也可抑制EGF的刺激作用。这些观察结果表明,从生物学和物理化学标准来看,成纤维细胞具有EGF受体,并表明血清中那些刺激细胞生长的因子中可能存在一种相似(如果不是相同)的肽。人们考虑了这样一种可能性,即EGF和霍乱毒素通过特定的细胞表面相互作用来调节细胞启动多核苷酸合成的能力,而这种相互作用反过来又会改变细胞内环磷酸腺苷的水平。

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