Induction of Autophagic Death in Cancer Cells by Agonizing TR3 and Attenuating Akt2 Activity.

Chemistry & biology Pub Date : 2015-08-20 Epub Date: 2015-07-30 DOI:10.1016/j.chembiol.2015.06.023

Wei-jia Wang, Yuan Wang, Pei-pei Hou, Feng-wei Li, Bo Zhou, Hang-zi Chen, Xue-li Bian, Qi-xu Cai, Yong-zhen Xing, Jian-ping He, Hongkui Zhang, Pei-qiang Huang, Tianwei Lin, Qiao Wu

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引用次数: 18

Abstract

Apoptotic resistance is becoming a significant obstacle for cancer therapy as the majority of treatment takes the route of apoptotic induction. It is of great importance to develop an alternative strategy to induce cancer cell death. We previously reported that autophagic cell death mediated by nuclear receptor TR3 and driven by a chemical agonist, 1-(3,4,5-trihydroxyphenyl)nonan-1-one (THPN), is highly effective in the therapy of melanoma but not any other cancer types. Here, we discovered that the insensitivity of cancer cells to THPN originated from a high cellular Akt2 activity. Akt2 phosphorylation interferes with TR3 export to cytoplasm and targeting to mitochondria, which lead to the autophagic induction. Therefore, the TR3-mediated autophagy could be effectively induced in the otherwise insensitive cells by downregulating Akt2 activity. Highly effective antineoplastic compounds are developed through optimizing the structure of THPN. This study implicates a general strategy for cancer therapy by the induction of autophagic cell death.

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通过诱导TR3和降低Akt2活性诱导癌细胞自噬死亡。

由于大多数肿瘤治疗采用诱导凋亡的途径，细胞凋亡耐药已成为肿瘤治疗的重要障碍。开发一种诱导癌细胞死亡的替代策略是非常重要的。我们之前报道过，由核受体TR3介导并由化学激动剂1-(3,4,5-三羟基苯基)nonan-1-one (THPN)驱动的自噬细胞死亡在治疗黑色素瘤中非常有效，但对任何其他类型的癌症无效。在这里，我们发现癌细胞对THPN的不敏感源于高细胞Akt2活性。Akt2磷酸化干扰TR3向细胞质输出并靶向线粒体，导致自噬诱导。因此，通过下调Akt2活性可以有效地诱导tr3介导的自噬。通过优化THPN的结构，开发出了高效的抗肿瘤化合物。这项研究暗示了通过诱导自噬细胞死亡来治疗癌症的一般策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Chemistry & biology 生物-生化与分子生物学

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审稿时长

4-8 weeks