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生长因子、v-Src 及终末分化对酪氨酸激酶底物 Eps8 表达的调控

Regulation of the tyrosine kinase substrate Eps8 expression by growth factors, v-Src and terminal differentiation.

作者信息

Gallo R, Provenzano C, Carbone R, Di Fiore P P, Castellani L, Falcone G, Alemà S

机构信息

Istituto di Biologia Cellulare, C.N.R., Roma, Italy.

出版信息

Oncogene. 1997 Oct 16;15(16):1929-36. doi: 10.1038/sj.onc.1201344.

Abstract

SH3-containing proteins are involved in signal transduction by a number of growth factor receptors and in the organization of the cytoskeleton. The recently identified Eps8 protein, which contains an SH3 domain, is coupled functionally and physically to the EGFR and is tyrosine phosphorylated by this receptor and other receptors as well. Here, we examined the regulation of eps8 expression in response to mitogenic or differentiative signals. We show that Eps8 is expressed at low levels in resting fibroblasts, but its expression is strongly induced during activation by serum, phorbol esters and the v-src oncogene. Conversely, expression of Eps8, but not of other EGFR substrates such as Shc or Eps15, is virtually extinguished in non-proliferating, terminally differentiated murine myogenic cells. The putative role of Eps8 protein as a v-Src substrate was analysed in murine fibroblasts and in quail myogenic cells expressing a temperature-sensitive variant of the tyrosine kinase. Tyrosine phosphorylation of Eps8 was detected only at the permissive temperature. A non-myristylated, transformation-defective mutant of v-Src did not phosphorylate Eps8, whereas it phosphorylated Shc. Together, these findings indicate that Eps8 may be a critical substrate of v-Src. They further establish Eps8 as an example of a signal transducer whose expression senses the balance between growth and differentiation and might, therefore, be involved in the determination of the phenotype.

摘要

含SH3结构域的蛋白质参与多种生长因子受体的信号转导以及细胞骨架的组织。最近鉴定出的Eps8蛋白含有一个SH3结构域,在功能和物理上与表皮生长因子受体(EGFR)偶联,并被该受体以及其他受体酪氨酸磷酸化。在此,我们研究了eps8表达对促有丝分裂或分化信号的响应调节。我们发现,Eps8在静止的成纤维细胞中低水平表达,但在血清、佛波酯和v-src癌基因激活过程中其表达被强烈诱导。相反,在非增殖、终末分化的小鼠成肌细胞中,Eps8的表达几乎消失,而其他EGFR底物如Shc或Eps15的表达则没有。在小鼠成纤维细胞和表达酪氨酸激酶温度敏感变体的鹌鹑成肌细胞中分析了Eps8蛋白作为v-Src底物的假定作用。仅在允许温度下检测到Eps8的酪氨酸磷酸化。v-Src的一种非肉豆蔻酰化、转化缺陷型突变体不能使Eps8磷酸化,而能使Shc磷酸化。这些发现共同表明,Eps8可能是v-Src的关键底物。它们进一步确立了Eps8作为信号转导分子的一个例子,其表达能感知生长与分化之间的平衡,因此可能参与表型的确定。

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