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Ribosomal protein S3: A multi-functional protein that interacts with both p53 and MDM2 through its KH domain.

机译:核糖体蛋白S3:一种多功能蛋白,可通过其KH结构域与p53和MDM2相互作用。

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摘要

The p53 protein responds to cellular stress and regulates genes involved in cell cycle, apoptosis, and DNA repair. Under normal conditions, p53 levels are kept low through MDM2-mediated ubiquitination and proteosomal degradation. In search for novel proteins that participate in this regulatory loop, we performed an MDM2 peptide pull-down assay and mass spectrometry to screen for potential interacting partners of MDM2. We identified ribosomal protein S3 (RPS3), whose interaction with MDM2, and notably p53, was further established by His and GST pull-down assays, fluorescence resonance energy transfer and an in situ proximity ligation assay. Additionally, in cells exposed to oxidative stress, p53 levels increased slightly over 24h, whereas MDM2 levels declined after 6h exposure, but rose over the next 18h of exposure. Conversely, in cells exposed to oxidative stress and harboring siRNA to knockdown RPS3 expression, decreased p53 levels and loss of the E3 ubiquitin ligase domain possessed by MDM2 were observed. DNA pull-down assays using a 7,8-dihydro-8-oxoguanine duplex oligonucleotide as a substrate found that RPS3 acted as a scaffold for the additional binding of MDM2 and p53, suggesting that RPS3 interacts with important proteins involved in maintaining genomic integrity.
机译:p53蛋白响应细胞压力并调节与细胞周期,细胞凋亡和DNA修复有关的基因。在正常条件下,p53水平通过MDM2介导的泛素化和蛋白体降解而保持较低水平。为了寻找参与此调节环的新型蛋白质,我们进行了MDM2肽下拉测定和质谱分析,以筛选MDM2的潜在相互作用伴侣。我们鉴定出了核糖体蛋白S3(RPS3),其与MDM2(尤其是p53)的相互作用是通过His和GST下拉测定,荧光共振能量转移和原位邻近结扎测定进一步建立的。此外,在暴露于氧化应激的细胞中,p53水平在24小时内略有增加,而MDM2水平在6h暴露后下降,但在接下来的18h升高。相反,在暴露于氧化应激并带有siRNA来敲低RPS3表达的细胞中,观察到MDM2拥有的p53水平降低和E3泛素连接酶结构域的丢失。使用7,8-二氢-8-氧鸟嘌呤双链体寡核苷酸作为底物的DNA下拉测定法发现RPS3充当MDM2和p53额外结合的支架,这表明RPS3与参与维持基因组完整性的重要蛋白质相互作用。

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