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GC选择性DNA结合抗生素光神霉素A揭示了Hdm2蛋白合成调控中的多个控制点。

GC-selective DNA-binding antibiotic, mithramycin A, reveals multiple points of control in the regulation of Hdm2 protein synthesis.

作者信息

Phillips A, Darley M, Blaydes J P

机构信息

Cancer Sciences Division, School of Medicine, University of Southampton, MP 824, Southampton General Hospital, Southampton, UK.

出版信息

Oncogene. 2006 Jul 13;25(30):4183-93. doi: 10.1038/sj.onc.1209451. Epub 2006 Feb 27.

Abstract

The primary role of the Hdm2/Mdm2 oncoprotein is to regulate the levels and activity of the transcription factor p53. Hdm2 synthesis is itself tightly controlled and, as demonstrated by a recently described SNP (SNP309) in the hdm2-P2 promoter, minor variations in Hdm2 expression have phenotypic consequences on radiation sensitivity and cancer predisposition. To further define mechanisms regulating Hdm2 expression, we have investigated the effects of the GC-selective DNA-binding drug, Mithramycin A (MA) on hdm2 mRNA transcription, trafficking, and translation. Firstly we show that the constitutive hdm2-P1 promoter is inhibited by MA. We define, for the first time, the minimal sequence elements that are required for P1-promoter activity and identify those which confer MA sensitivity. Secondly, MA induces p53-dependent transcription from the hdm2-P2 promoter. Thirdly, and critically, MA also inhibits Hdm2 synthesis at the post-transcriptional level, with negative effects on hdm2 mRNA nuclear export and translation. This study highlights the complex interplay between the pathways that regulate Hdm2 protein synthesis in cancer cells, and furthermore emphasizes the export of hdm2 mRNA from the nucleus to the cytoplasm as a key point of control in this process.

摘要

Hdm2/Mdm2癌蛋白的主要作用是调节转录因子p53的水平和活性。Hdm2的合成本身受到严格控制,正如最近在hdm2 - P2启动子中描述的一个单核苷酸多态性(SNP309)所表明的那样,Hdm2表达的微小变化对辐射敏感性和癌症易感性具有表型影响。为了进一步确定调节Hdm2表达的机制,我们研究了GC选择性DNA结合药物光神霉素A(MA)对hdm2 mRNA转录、运输和翻译的影响。首先,我们发现组成型hdm2 - P1启动子受到MA的抑制。我们首次确定了P1启动子活性所需的最小序列元件,并确定了赋予MA敏感性的元件。其次,MA诱导hdm2 - P2启动子的p53依赖性转录。第三,也是至关重要的一点,MA还在转录后水平抑制Hdm2的合成,对hdm2 mRNA的核输出和翻译产生负面影响。这项研究突出了癌细胞中调节Hdm2蛋白合成的途径之间复杂的相互作用,并且进一步强调了hdm2 mRNA从细胞核输出到细胞质是这一过程中的一个关键控制点。

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