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v-Src通过Ras-MAP激酶途径抑制SHPS-1的表达,以促进细胞的致癌生长。

v-Src suppresses SHPS-1 expression via the Ras-MAP kinase pathway to promote the oncogenic growth of cells.

作者信息

Machida K, Matsuda S, Yamaki K, Senga T, Thant A A, Kurata H, Miyazaki K, Hayashi K, Okuda T, Kitamura T, Hayakawa T, Hamaguchi M

机构信息

Department of Molecular Pathogenesis, Nagoya University School of Medicine, Japan.

出版信息

Oncogene. 2000 Mar 23;19(13):1710-8. doi: 10.1038/sj.onc.1203497.

Abstract

We investigated the effect of cell transformation by v-src on the expression and tyrosine phosphorylation of SHPS-1, a putative docking protein for SHP-1 and SHP-2. We found that transformation by v-src virtually inhibited the SHPS-1 expression at mRNA level. While nontransforming Src kinases including c-Src, nonmyristoylated forms of v-Src had no inhibitory effect on SHPS-1 expression, transforming Src kinases including wild-type v-Src and chimeric mutant of c-Src bearing v-Src SH3 substantially suppressed the SHPS-1 expression. In cells expressing temperature sensitive mutant of v-Src, suppression of the SHPS-1 expression was temperature-dependent. In contrast, tyrosine phosphorylation of SHPS-1 was rather activated in cells expressing c-Src or nonmyristoylated forms of v-Src. SHPS-1 expression in SR3Y1 was restored by treatment with herbimycin A, a potent inhibitor of tyrosine kinase, or by the expression of dominant negative form of Ras. Contrary, active form of Mekl markedly suppressed SHPS-1 expression. Finally, overexpression of SHPS-1 in SR3Y1 led to the drastic reduction of anchorage independent growth of the cells. Taken together, our results suggest that the suppression of SHPS-1 expression is a pivotal event for cell transformation by v-src, and the Ras-MAP kinase cascade plays a critical role in the suppression.

摘要

我们研究了v-src介导的细胞转化对SHPS-1表达及酪氨酸磷酸化的影响,SHPS-1是一种推测的SHP-1和SHP-2对接蛋白。我们发现,v-src介导的转化在mRNA水平上几乎抑制了SHPS-1的表达。虽然包括c-Src在内的非转化型Src激酶、v-Src的非肉豆蔻酰化形式对SHPS-1表达没有抑制作用,但包括野生型v-Src和携带v-Src SH3的c-Src嵌合突变体在内的转化型Src激酶则显著抑制了SHPS-1的表达。在表达v-Src温度敏感突变体的细胞中,SHPS-1表达的抑制具有温度依赖性。相反,在表达c-Src或v-Src非肉豆蔻酰化形式的细胞中,SHPS-1的酪氨酸磷酸化反而被激活。用酪氨酸激酶强效抑制剂赫伯霉素A处理或表达显性负性形式的Ras可恢复SR3Y1细胞中SHPS-1的表达。相反,活性形式的Mek1显著抑制SHPS-1的表达。最后,在SR3Y1细胞中过表达SHPS-1导致细胞锚定非依赖性生长急剧减少。综上所述,我们的结果表明,抑制SHPS-1表达是v-src介导细胞转化的关键事件,且Ras-MAP激酶级联反应在该抑制过程中起关键作用。

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