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Cooperation between the ribosomal proteins L5 and L11 in the p53 pathway

机译:核糖体蛋白L5和L11在p53途径中的合作

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MDM2 is a ubiquitin ligase that plays a key role in regulating the stability of the p53 tumor suppressor protein. Several proteins have been shown to activate the p53 pathway by interacting with and inhibiting the E3 function of MDM2, thereby leading to an accumulation of p53. These include the alternate reading frame (ARF) proteins and the ribosomal proteins L5 and L11. We found that when overexpressed alone, L11 is much less potent in inhibiting MDM2 than p14ARF. However, L11 cooperates with L5, resulting in a robust inhibition of the E3 activity of MDM2, and a stabilization and activation of p53 approaching that achieved by p14ARF. We further showed that the ability of L11 to bind the 5S rRNA is important for the cooperation with L5, and a mutant L11, which cannot bind the 5S rRNA, cannot cooperate with L5 in inhibiting MDM2.
机译:MDM2是一种泛素连接酶,在调节p53肿瘤抑制蛋白的稳定性中起关键作用。已显示出几种蛋白质通过与MDM2相互作用并抑制其功能,从而激活p53途径,从而导致p53的积累。这些包括替代阅读框(ARF)蛋白和核糖体蛋白L5和L11。我们发现,当单独过度表达时,L11抑制MDM2的能力远低于p14ARF。但是,L11与L5协同作用,导致对MDM2的E3活性的强烈抑制,并使p53的稳定和活化接近p14ARF所达到的水平。我们进一步表明,L11结合5S rRNA的能力对于与L5的合作非常重要,而不能结合5S rRNA的突变体L11不能与L5协同抑制MDM2。

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