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在潜在信号模块中,c-N-Ras与c-Raf-1和蛋白激酶Cε的组成型关联。

Constitutive association of c-N-Ras with c-Raf-1 and protein kinase C epsilon in latent signaling modules.

作者信息

Hamilton M, Liao J, Cathcart M K, Wolfman A

机构信息

Department of Cell Biology, The Lerner Research Institute, Cleveland Clinic Foundation, Cleveland, Ohio 44195, USA.

出版信息

J Biol Chem. 2001 Aug 3;276(31):29079-90. doi: 10.1074/jbc.M102001200. Epub 2001 May 17.

Abstract

Phorbol ester stimulation of the MAPK cascade is believed to be mediated through the protein kinase C (PKC)-dependent activation of Raf-1. Although several studies suggest that phorbol ester stimulation of MAPK is insensitive to dominant-negative Ras, a requirement for Ras in Raf-1 activation by PKC has been suggested recently. We now demonstrate that in normal, quiescent mouse fibroblasts, endogenous c-N-Ras is constitutively associated with both c-Raf-1 and PKC epsilon in a biochemically silent, but latent, signaling module. Chemical inhibition of novel PKCs blocks phorbol 12-myristate 13-acetate (PMA)-mediated activation of MAPKs. Down-regulation of PKC epsilon protein levels by antisense oligodeoxyribonucleotides blocks MAPK activation in response to PMA stimulation, demonstrating that PKC epsilon activity is required for MAPK activation by PMA. c-Raf-1 activity in immunoprecipitated c-N-Ras.c-Raf-1.PKC epsilon complexes is stimulated by PMA and is inhibited by GF109203X, thereby linking c-Raf-1 activation in this complex to PKC activation. These observations suggest that in quiescent cells Ras is organized into ordered, inactive signaling modules. Furthermore, the regulation of the MAPK cascade by both Ras and PKC is intimately linked, converging at the plasma membrane through their association with c-Raf-1.

摘要

佛波酯对丝裂原活化蛋白激酶(MAPK)级联反应的刺激作用被认为是通过蛋白激酶C(PKC)依赖的Raf-1激活来介导的。尽管多项研究表明佛波酯对MAPK的刺激作用对显性负性Ras不敏感,但最近有人提出在PKC激活Raf-1的过程中Ras是必需的。我们现在证明,在正常的、静止的小鼠成纤维细胞中,内源性c-N-Ras在一个生化沉默但潜在的信号模块中与c-Raf-1和PKCε持续相关。对新型PKC的化学抑制可阻断佛波酯12-肉豆蔻酸酯13-乙酸酯(PMA)介导的MAPK激活。反义寡脱氧核苷酸下调PKCε蛋白水平可阻断对PMA刺激的MAPK激活,表明PKCε活性是PMA激活MAPK所必需的。免疫沉淀的c-N-Ras.c-Raf-1.PKCε复合物中的c-Raf-1活性受到PMA的刺激,并被GF109203X抑制,从而将该复合物中c-Raf-1的激活与PKC激活联系起来。这些观察结果表明,在静止细胞中,Ras被组织成有序的、无活性的信号模块。此外,Ras和PKC对MAPK级联反应的调节密切相关,通过它们与c-Raf-1的结合在质膜处汇聚。

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