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本文引用的文献

1
FOXOs, cancer and regulation of apoptosis.叉头框蛋白O(FOXOs)、癌症与细胞凋亡调控
Oncogene. 2008 Apr 7;27(16):2312-9. doi: 10.1038/onc.2008.24.
2
Histone deacetylase inhibitor depsipeptide activates silenced genes through decreasing both CpG and H3K9 methylation on the promoter.组蛋白去乙酰化酶抑制剂缩酚酸肽通过降低启动子上的CpG和H3K9甲基化来激活沉默基因。
Mol Cell Biol. 2008 May;28(10):3219-35. doi: 10.1128/MCB.01516-07. Epub 2008 Mar 10.
3
Fas Bim boom!Fas、Bim ,迅速发展! (注:由于文本简短且含义不明,这样翻译可能不太符合医学专业语境,仅按字面翻译,可能需要更多上下文来准确理解其确切意思)
Immunity. 2008 Feb;28(2):141-3. doi: 10.1016/j.immuni.2008.01.004.
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Histone deacetylase inhibitors: molecular mechanisms of action.组蛋白去乙酰化酶抑制剂:作用的分子机制
Oncogene. 2007 Aug 13;26(37):5541-52. doi: 10.1038/sj.onc.1210620.
5
Dynamic FoxO transcription factors.动态FoxO转录因子
J Cell Sci. 2007 Aug 1;120(Pt 15):2479-87. doi: 10.1242/jcs.001222.
6
Transcriptional regulation of Bim by FoxO3A mediates hepatocyte lipoapoptosis.FoxO3A对Bim的转录调控介导肝细胞脂肪凋亡。
J Biol Chem. 2007 Sep 14;282(37):27141-27154. doi: 10.1074/jbc.M704391200. Epub 2007 Jul 11.
7
Apoptosis induced by histone deacetylase inhibitors in leukemic cells is mediated by Bim and Noxa.组蛋白脱乙酰酶抑制剂诱导白血病细胞凋亡是由Bim和Noxa介导的。
Leukemia. 2007 Aug;21(8):1773-82. doi: 10.1038/sj.leu.2404760. Epub 2007 May 24.
8
Stressing the role of FoxO proteins in lifespan and disease.强调FoxO蛋白在寿命和疾病中的作用。
Nat Rev Mol Cell Biol. 2007 Jun;8(6):440-50. doi: 10.1038/nrm2190.
9
Forkhead proteins are critical for bone morphogenetic protein-2 regulation and anti-tumor activity of resveratrol.叉头蛋白对于骨形态发生蛋白-2的调节以及白藜芦醇的抗肿瘤活性至关重要。
J Biol Chem. 2007 Jul 6;282(27):19385-98. doi: 10.1074/jbc.M702452200. Epub 2007 May 18.
10
Analysis of the apoptotic and therapeutic activities of histone deacetylase inhibitors by using a mouse model of B cell lymphoma.利用B细胞淋巴瘤小鼠模型分析组蛋白去乙酰化酶抑制剂的凋亡和治疗活性。
Proc Natl Acad Sci U S A. 2007 May 8;104(19):8071-6. doi: 10.1073/pnas.0702294104. Epub 2007 Apr 30.

FoxO1的乙酰化激活Bim表达,以响应组蛋白去乙酰化酶抑制剂缩肽素治疗诱导细胞凋亡。

Acetylation of FoxO1 activates Bim expression to induce apoptosis in response to histone deacetylase inhibitor depsipeptide treatment.

作者信息

Yang Yang, Zhao Ying, Liao Wenjuan, Yang Jing, Wu Lipeng, Zheng Zhixing, Yu Yu, Zhou Wen, Li Lian, Feng Jingnan, Wang Haiying, Zhu Wei-Guo

机构信息

Key Laboratory of Carcinogenesis and Translational Research (Ministry of Education), Department of Biochemistry and Molecular Biology, Peking University Health Science Center, #38 Xueyuan Road, Beijing 100191, China.

出版信息

Neoplasia. 2009 Apr;11(4):313-24. doi: 10.1593/neo.81358.

DOI:10.1593/neo.81358
PMID:19308286
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2657887/
Abstract

Histone deacetylase (HDAC) inhibitors have been shown to induce cell cycle arrest and apoptosis in cancer cells. However, the mechanisms of HDAC inhibitor induced apoptosis are incompletely understood. In this study, depsipeptide, a novel HDAC inhibitor, was shown to be able to induce significant apoptotic cell death in human lung cancer cells. Further study showed that Bim, a BH3-only proapoptotic protein, was significantly upregulated by depsipeptide in cancer cells, and Bim's function in depsipeptide-induced apoptosis was confirmed by knockdown of Bim with RNAi. In addition, we found that depsipeptide-induced expression of Bim was directly dependent on acetylation of forkhead box class O1 (FoxO1) that is catalyzed by cyclic adenosine monophosphate-responsive element-binding protein-binding protein, and indirectly induced by a decreased four-and-a-half LIM-domain protein 2. Moreover, our results demonstrated that FoxO1 acetylation is required for the depsipeptide-induced activation of Bim and apoptosis, using transfection with a plasmid containing FoxO1 mutated at lysine sites and a luciferase reporter assay. These data show for the first time that an HDAC inhibitor induces apoptosis through the FoxO1 acetylation-Bim pathway.

摘要

组蛋白去乙酰化酶(HDAC)抑制剂已被证明可诱导癌细胞的细胞周期停滞和凋亡。然而,HDAC抑制剂诱导凋亡的机制尚未完全明确。在本研究中,新型HDAC抑制剂缩肽被证明能够在人肺癌细胞中诱导显著的凋亡性细胞死亡。进一步研究表明,仅含BH3结构域的促凋亡蛋白Bim在癌细胞中被缩肽显著上调,并且通过RNA干扰敲低Bim证实了其在缩肽诱导凋亡中的作用。此外,我们发现缩肽诱导的Bim表达直接依赖于由环磷酸腺苷反应元件结合蛋白结合蛋白催化的叉头框O1类(FoxO1)的乙酰化,并间接由四又二分之一LIM结构域蛋白2的减少所诱导。此外,我们的结果表明,使用含有在赖氨酸位点突变的FoxO1的质粒转染和荧光素酶报告基因检测,FoxO1乙酰化是缩肽诱导Bim激活和凋亡所必需的。这些数据首次表明HDAC抑制剂通过FoxO1乙酰化 - Bim途径诱导凋亡。