首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Artemisinin Blocks Prostate Cancer Growth and Cell Cycle Progression by Disrupting Sp1 Interactions with the Cyclin-dependent Kinase-4 (CDK4) Promoter and Inhibiting CDK4 Gene Expression

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Artemisinin Blocks Prostate Cancer Growth and Cell Cycle Progression by Disrupting Sp1 Interactions with the Cyclin-dependent Kinase-4 (CDK4) Promoter and Inhibiting CDK4 Gene Expression

机译：青蒿素阻止前列腺癌的生长和细胞周期的进展破坏与细胞周期蛋白依赖性激酶4（CDK4）启动子的Sp1相互作用。和抑制CDK4基因表达

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Artemisinin, a naturally occurring component of Artemisia annua, or sweet wormwood, is a potent anti-malaria compound that has recently been shown to have anti-proliferative effects on a number of human cancer cell types, although little is know about the molecular mechanisms of this response. We have observed that artemisinin treatment triggers a stringent G1 cell cycle arrest of LNCaP (lymph node carcinoma of the prostate) human prostate cancer cells that is accompanied by a rapid down-regulation of CDK2 and CDK4 protein and transcript levels. Transient transfection with promoter-linked luciferase reporter plasmids revealed that artemisinin strongly inhibits CDK2 and CDK4 promoter activity. Deletion analysis of the CDK4 promoter revealed a 231-bp artemisinin-responsive region between -1737 and -1506. Site-specific mutations revealed that the Sp1 site at -1531 was necessary for artemisinin responsiveness in the context of the CDK4 promoter. DNA binding assays as well as chromatin immunoprecipitation assays demonstrated that this Sp1-binding site in the CDK4 promoter forms a specific artemisinin-responsive DNA-protein complex that contains the Sp1 transcription factor. Artemisinin reduced phosphorylation of Sp1, and when dephosphorylation of Sp1 was inhibited by treatment of cells with the phosphatase inhibitor okadaic acid, the ability of artemisinin to down-regulate Sp1 interactions with the CDK4 promoter was ablated, rendering the CDK4 promoter unresponsive to artemisinin. Finally, overexpression of Sp1 mostly reversed the artemisinin down-regulation of CDK4 promoter activity and partially reversed the cell cycle arrest. Taken together, our results demonstrate that a key event in the artemisinin anti-proliferative effects in prostate cancer cells is the transcriptional down-regulation of CDK4 expression by disruption of Sp1 interactions with the CDK4 promoter.

机译：青蒿素是青蒿的天然成分，它是一种有效的抗疟疾化合物，最近被证实对多种人类癌细胞具有抗增殖作用，尽管对其的分子机制了解甚少。这个回应。我们已经观察到青蒿素治疗触发LNCaP（前列腺淋巴结癌）人前列腺癌细胞的严格G1细胞周期停滞，并伴有CDK2和CDK4蛋白及转录水平的快速下调。用启动子连接的荧光素酶报告质粒瞬时转染显示青蒿素强烈抑制CDK2和CDK4启动子活性。 CDK4启动子的缺失分析表明，在-1737和-1506之间有一个231 bp的青蒿素响应区域。位点特异性突变表明，在CDK4启动子的背景下，-1531处的Sp1位点对于青蒿素的响应是必需的。 DNA结合测定以及染色质免疫沉淀测定表明，CDK4启动子中的Sp1结合位点形成了一个特定的青蒿素反应性DNA-蛋白质复合物，其中含有Sp1转录因子。青蒿素减少Sp1的磷酸化以及去磷酸化时 Sp1的表达被磷酸酶抑制剂所抑制冈田酸，青蒿素下调Sp1相互作用的能力去除了带有CDK4启动子的CDK4启动子青蒿素。最后，Sp1的过表达主要逆转了青蒿素下调CDK4启动子活性并部分逆转细胞循环逮捕。综上所述，我们的结果表明，青蒿素在前列腺癌细胞中的抗增殖作用是转录下调Sp1破坏CDK4表达。与CDK4启动子的相互作用。

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期刊名称 The Journal of Biological Chemistry
作者
Jamin A. Willoughby Sr.; Shyam N. Sundar; Mark Cheung; Antony S. Tin; Jaime Modiano; Gary L. Firestone;
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年(卷),期 2009(284),4
年度 2009
页码 2203–2213
总页数 11
原文格式 PDF
正文语种
中图分类分子生物学;
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1. Artemisinin triggers a G1 cell cycle arrest of human Ishikawa endometrial cancer cells and inhibits cyclin-dependent kinase-4 promoter activity and expression by disrupting nuclear factor-κB transcriptional signaling [J] . TranK.Q., TinA.S., FirestoneG.L. Anti-cancer drugs . 2014,第3期

机译：青蒿素触发Ishikawa子宫内膜癌细胞的G1细胞周期阻滞，并通过破坏核因子κB转录信号传导来抑制细胞周期蛋白依赖性激酶4启动子活性和表达。
2. Release from cell cycle arrest with Cdk4/6 inhibitors generates highly synchronized cell cycle progression in human cell culture [J] . Eleanor Wendy Trotter, Iain Michael Hagan Open Biology . 2020,第10期

机译：通过CDK4 / 6抑制剂从细胞周期停滞中释放，在人细胞培养中产生高度同步的细胞周期进展
3. Soy milk digestion extract inhibits progression of prostate cancer cell growth via regulation of prostate cancer-specific antigen and cell cycle-regulatory genes in human LNCaP cancer cells [J] . Kang Nam-Hee, Shin Hee-Chang, Oh Seunghyun, Molecular medicine reports . 2016,第2aPta1期

机译：豆浆消化提取物通过调节人LNCaP癌细胞中的前列腺癌特异性抗原和细胞周期调控基因来抑制前列腺癌细胞生长的进程
4. A Mixed-micellar siRNA Delivery System for Gene Specific Cancer Therapeutics by a Synthetic Lethal Interaction Between KRAS Cdk4 [C] . Cheng-Qiong Mao, Meng-Hua Xiong, Jun Wang World biomaterials congress . 2012

机译：KRAS与Cdk4之间的合成致死相互作用的混合胶束siRNA递送系统，用于基因特异性癌症治疗。
5. Identification of Genomic Predictors of Response to the CDK4/6 Inhibitor Palbociclib using the UCLATORL Panel of Human Cancer Cell Lines [D] . Conklin, Dylan Francis 2013

机译：使用人类癌细胞系UCLATORL小组鉴定对CDK4 / 6抑制剂Palbociclib应答的基因组预测因子
6. Artemisinin triggers a G1 cell cycle arrest of human Ishikawa endometrial cancer cells and inhibits Cyclin Dependent Kinase-4 promoter activity and expression by disrupting NF-kB transcriptional signaling [O] . Kalvin Q. Tran, Antony S. Tin, Gary L. Firestone -1

机译：青蒿素触发人Ishikawa子宫内膜癌细胞的G1细胞周期阻滞并通过破坏NF-kB转录信号传导抑制细胞周期蛋白依赖性激酶4启动子的活性和表达。
7. Artemisinin Blocks Prostate Cancer Growth and Cell Cycle Progression by Disrupting Sp1 Interactions with the Cyclin-dependent Kinase-4 (CDK4) Promoter and Inhibiting CDK4 Gene Expression* [O] . Willoughby, Jamin A., Sundar, Shyam N., Cheung, Mark, 2008

机译：青蒿素阻止前列腺癌的生长和细胞周期的进展破坏与细胞周期蛋白依赖性激酶4（CDK4）启动子的Sp1相互作用。和抑制CDK4基因表达*

Artemisinin Blocks Prostate Cancer Growth and Cell Cycle Progression by Disrupting Sp1 Interactions with the Cyclin-dependent Kinase-4 (CDK4) Promoter and Inhibiting CDK4 Gene Expression

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