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表皮生长因子受体功能的第二信使调节并非发生在受体二聚化水平。

Second messenger modulation of epidermal growth factor receptor function does not occur at the level of receptor dimerization.

作者信息

Verheijden G F, Verlaan I, van Iersel M J, Moolenaar W H

机构信息

Division of Cellular Biochemistry, Netherlands Cancer Institute, Amsterdam.

出版信息

Biochem J. 1990 Oct 1;271(1):215-21. doi: 10.1042/bj2710215.

Abstract

Epidermal growth factor (EGF)-induced receptor dimerization may provide a mechanism for activation of the receptor protein tyrosine kinase and for initiation of post-receptor signalling pathways. We have examined whether second messengers and agents that modulate EGF receptor function act at the level of receptor dimerization. Both the Ca2+ ionophore ionomycin and the tumour promotor tetradecanoylphorbol acetate (TPA), added shortly before EGF, inhibit EGF receptor protein tyrosine kinase activity in intact cells. In permeabilized cells, elevation of Ca2+ similarly inhibits EGF receptor function. The inhibitory effect of Ca2+, unlike that of TPA, appears not to be dependent on protein kinase C activity. Neither ionomycin nor phorbol ester affects EGF-induced receptor dimerization, as shown by cross-linking and immunoblotting techniques, although the phosphotyrosine content of both monomeric and dimeric receptors is strongly decreased. Furthermore, we show that EGF receptor dimerization is not affected by increases in cyclic AMP or intracellular pH, nor by changes in transmembrane potential, medium osmolarity or the glycosylation state of the receptor. These result suggest that modulation of EGF receptor function occurs at a step other than receptor dimerization.

摘要

表皮生长因子(EGF)诱导的受体二聚化可能为受体蛋白酪氨酸激酶的激活以及受体后信号通路的启动提供一种机制。我们研究了第二信使和调节EGF受体功能的试剂是否在受体二聚化水平起作用。在EGF加入前不久添加的钙离子载体离子霉素和肿瘤促进剂十四酰佛波醇乙酸酯(TPA),均可抑制完整细胞中EGF受体蛋白酪氨酸激酶活性。在通透细胞中,钙离子浓度升高同样会抑制EGF受体功能。与TPA不同,钙离子的抑制作用似乎不依赖于蛋白激酶C活性。交联和免疫印迹技术表明,离子霉素和佛波酯均不影响EGF诱导的受体二聚化,尽管单体和二聚体受体的磷酸酪氨酸含量均显著降低。此外,我们发现EGF受体二聚化不受环磷酸腺苷或细胞内pH升高的影响,也不受跨膜电位、培养基渗透压或受体糖基化状态变化的影响。这些结果表明,EGF受体功能的调节发生在受体二聚化之外的步骤。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ca68/1149535/b54e6ff6dbb0/biochemj00174-0205-a.jpg

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