高葡萄糖使丝氨酸 46 去磷酸化并抑制 p53 的凋亡活性。

High glucose dephosphorylates serine 46 and inhibits p53 apoptotic activity.

出版信息

J Exp Clin Cancer Res. 2014 Sep 27;33(1):79. doi: 10.1186/s13046-014-0079-4.

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4181716/

Abstract

BACKGROUND

In response to diverse genotoxic stimuli p53 is activated as transcription factor to exert its tumor-suppressor function. P53 activation requires protein stabilization, nuclear localization and posttranslational modifications in key residues that may influence p53 selection of target genes. Among them, serine 46 (Ser46) phosphorylation is considered specific for apoptotic activation. Hyperglicaemia, the high blood glucose condition, may negatively affect tumor response to therapies through several mechanisms, conferring resistance to drug-induced cell death. However, whether high glucose might modify p53Ser46 phosphorylation has never been addressed.

METHODS AND RESULTS

Here, we performed biochemical and molecular analyses in different cancer cell lines treated with chemotherapy in the presence or absence of high glucose condition. Analyses of p53 posttranslational modifications showed that drug-induced p53Ser46 phosphorylation was reduced by high glucose. Such reduction depended by high glucose-induced calyculin A-sensitive phosphatase(s), able to specifically target p53Ser46 phosphorylation. The specific effect on Ser46 phosphorylation was addressed by analysing Ser15 phosphorylation that instead was not modified by high glucose. In agreement, a constitutively phosphorylated Ser46D p53 mutant was resistant to high glucose. As a consequence of phosphoSer46 impairment, high glucose reduced the tumor cell response to drugs, correlating with reduced p53 apoptotic transactivation. The drug-induced apoptotic cell death, reduced by high glucose, was finally restored by the phosphatase inhibitor calyculin A.

CONCLUSIONS

These data indicate that high glucose specifically inhibited Ser46 phosphorylation thus reducing p53 apoptotic activity. These results uncover a new mechanism of p53 inactivation providing an interesting novel molecular link between metabolic diseases such as diabetes or obesity and tumor progression and resistance to therapies.

摘要

背景

为应对各种遗传毒性刺激，p53 作为转录因子被激活，发挥其肿瘤抑制功能。p53 的激活需要蛋白质稳定、核定位以及关键残基的翻译后修饰，这些修饰可能会影响 p53 对靶基因的选择。其中，丝氨酸 46（Ser46）磷酸化被认为是凋亡激活的特异性标志。高血糖（血液中葡萄糖含量过高）可能通过多种机制对肿瘤的治疗反应产生负面影响，导致对药物诱导的细胞死亡产生抵抗。然而，高血糖是否会改变 p53Ser46 磷酸化尚未得到证实。

方法和结果

在此，我们在不同的癌细胞系中进行了生化和分子分析，这些细胞系在存在或不存在高葡萄糖条件下接受了化疗。p53 翻译后修饰分析表明，高葡萄糖降低了药物诱导的 p53Ser46 磷酸化。这种降低依赖于高葡萄糖诱导的 calyculin A 敏感磷酸酶（phosphatase），其能够特异性靶向 p53Ser46 磷酸化。通过分析 Ser15 磷酸化（其未受高葡萄糖影响）来确定 Ser46 磷酸化的特异性。相反，组成性磷酸化 Ser46D p53 突变体对高葡萄糖具有抗性。由于 Ser46 磷酸化受损，高葡萄糖降低了肿瘤细胞对药物的反应，这与 p53 凋亡转录激活减少有关。高葡萄糖降低的药物诱导的凋亡细胞死亡最终通过磷酸酶抑制剂 calyculin A 得到恢复。

结论

这些数据表明，高葡萄糖特异性抑制了 Ser46 磷酸化，从而降低了 p53 的凋亡活性。这些结果揭示了 p53 失活的一种新机制，为代谢性疾病（如糖尿病或肥胖症）与肿瘤进展和治疗抵抗之间提供了一个有趣的新的分子联系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d135/4181716/33c982ba39be/13046_2014_79_Fig1_HTML.jpg

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高葡萄糖使丝氨酸 46 去磷酸化并抑制 p53 的凋亡活性。

High glucose dephosphorylates serine 46 and inhibits p53 apoptotic activity.

出版信息

BACKGROUND

METHODS AND RESULTS

CONCLUSIONS

背景

方法和结果

结论

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