活化的新受体酪氨酸激酶诱导的细胞血小板衍生生长因子受体的下调。

L Lehtola, M Nistér, E Hölttä, B Westermark, K Alitalo
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引用次数: 4

摘要

生长因子信号的功能整合发生在靶细胞的几个水平上。最接近的机制之一是受体转调,通过这种机制,一个激活的受体可以调节同一细胞中其他受体的表达。已建立的跨调节回路涉及血小板源性生长因子(PDGF)对表皮生长因子(EGF)受体的下调和β型转化生长因子对PDGF受体的调节。我们在转染的NIH/3T3细胞中研究了新酪氨酸激酶活化与PDGF受体表达的关系。通过[125- 1]PDGF- aa和- bb结合测量,新癌基因的表达,而不是新原癌基因的表达,与细胞表面PDGF α和β受体的减少有关。这些结果被代谢标记和PDGF β受体的免疫沉淀证实。与表达新原癌基因的对照细胞相比,PDGF α和β受体mrna在新癌基因转化的细胞中明显减少。在EGF处理表达嵌合EGF受体/新受体的细胞后,也观察到PDGF受体及其mrna的下调,其中新酪氨酸激酶被EGF结合激活。上述结果表明,新型酪氨酸激酶可以下调PDGF受体的表达,其作用机制可能是通过降低PDGF受体mRNA水平介导的。
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Down-regulation of cellular platelet-derived growth factor receptors induced by an activated neu receptor tyrosine kinase.

The functional integration of growth factor signaling occurs at several levels in target cells. One of the most proximal mechanisms is receptor transmodulation, by which one activated receptor can regulate the expression of other receptors in the same cells. Well-established transregulatory loops involve platelet-derived growth factor (PDGF) down-regulation of epidermal growth factor (EGF) receptors and beta-type transforming growth factors modulation of PDGF receptors. We have studied the relationship between neu tyrosine kinase activation and the expression of the PDGF receptors in transfected NIH/3T3 cells. Expression of the neu oncogene, but not of the neu proto-oncogene, was associated with a decrease of PDGF alpha- and beta-receptors on the cell surface, as measured by [125-I]PDGF-AA and -BB binding. These results were corroborated by metabolic labeling and immunoprecipitation of the PDGF beta-receptors. PDGF alpha- and beta-receptor mRNAs were strongly decreased in the neu oncogene-transformed cells in comparison with control cells expressing the neu proto-oncogene. Down-regulation of the PDGF receptors and their mRNAs was also observed after EGF treatment of cells expressing a chimeric EGF receptor/neu receptor, where the neu tyrosine kinase is activated by EGF binding. These results show that the neu tyrosine kinase can down-modulate PDGF receptor expression, and the effect is mediated via decreased PDGF receptor mRNA levels.

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