首页> 外文期刊>The Journal of biological chemistry >Dynamic Ubiquitination of the Mitogen-activated Protein Kinase Kinase (MAPKK) Ste7 Determines Mitogen-activated Protein Kinase (MAPK) Specificity
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Dynamic Ubiquitination of the Mitogen-activated Protein Kinase Kinase (MAPKK) Ste7 Determines Mitogen-activated Protein Kinase (MAPK) Specificity

机译:丝裂原激活蛋白激酶激酶(MAPKK)STE7的动态泛素测定丝裂原活化蛋白激酶(MAPK)特异性

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Ubiquitination is a post-translational modification that tags proteins for proteasomal degradation. In addition, there is a growing appreciation that ubiquitination can influence protein activity and localization. Ste7 is a prototype MAPKK in yeast that participates in both the pheromone signaling and nutrient deprivation/invasive growth pathways. We have shown previously that Ste7 is ubiquitinated upon pheromone stimulation. Here, we show that the Skp1/Cullin/F-box ubiquitin ligase SCFCdc4 and the ubiquitin protease Ubp3 regulate Ste7 ubiquitination and signal specificity. Using purified components, we demonstrate that SCFCdc4 ubiquitinates Ste7 directly. Using gene deletion mutants, we show that SCFCdc4 and Ubp3 have opposing effects on Ste7 ubiquitination. Although SCFCdc4 is necessary for proper activation of the pheromone MAPK Fus3, Ubp3 is needed to limit activation of the invasive growth MAPK Kss1. Finally, we show that Fus3 phosphorylates Ubp3 directly and that phosphorylation of Ubp3 is necessary to limit Kss1 activation. These results reveal a feedback loop wherein one MAPK limits the ubiquitination of an upstream MAPKK and thereby prevents spurious activation of a second competing MAPK.
机译:泛素化是翻译后修饰,其标记蛋白质进行蛋白酶体降解。此外,普遍存在的升值越来越大,可以影响蛋白质活性和局部化。 STE7是酵母的原型MAPKK,参与信息素信号和营养剥夺/侵袭性生长途径。我们以前表明,STE7在信息素刺激时染上了STE7。在这里,我们表明SKP1 / Cullin / F箱泛素连接酶SCFCDC4和泛素蛋白酶UBP3调节STE7 ubiquitatch和信号特异性。使用纯化的组分,我们证明SCFCDC4直接突出了STE7。使用基因缺失突变体,我们表明SCFCDC4和UBP3对STE7泛素化的反对作用。尽管SCFCDC4是正确激活信息素MAPK FUS3的必要条件,但需要UBP3来限制侵入性生长MAPK KSS1的激活。最后,我们表明Fus3直接磷酸化UBP3,并且UBP3的磷酸化是限制KSS1活化的必要条件。这些结果揭示了一种反馈循环,其中一个MAPK限制了上游MAPKK的泛素,从而防止了第二个竞争MAPK的虚假激活。

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