CyclinD1 protein plays different roles in modulating chemoresponses in MCF7 and MDA-MB231 cells.

Q1 Environmental Science

Journal of Carcinogenesis Pub Date : 2012-01-01 Epub Date: 2012-08-30 DOI:10.4103/1477-3163.100401

Yuan Sun, Dianzhong Luo, D Joshua Liao

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引用次数: 30

Abstract

Background: CyclinD1 is an essential sensor and activator of cell cycle initiation and progression; overexpression of cyclinD1 is linked to various human cancers, including breast cancer. The elevated cyclinD1 in some types of cancers is believed to be associated with tumor progression and response to systemic treatments.

Aims: In this study, we anticipate to address the questions in human breast cancer; the function of cyclinD1 in mediating chemoresponses; and the signaling pathway cooperating with cyclinD1 to interfere with the drug functions.

Materials and methods: Using the cell clones, concurrent ectopic expression of the wild-type or K112E-mutated human cyclinD1 protein in the MCF7 and MDA-MB231 (MB231) breast cancer cells to study the function of cyclinD1 in responses to the chemotherapeutic treatments. Three drugs, cisplatin (CDDP), 5-fluorouracil (5-FU), and Gemzar were used in this study; the 3-(4,5-dimethylthiazol-2-yl)-2, 5-diphenyltetrazolium bromide (MTT) assay, cell cycle and cell death analysis, clonogenic survival assay, acridine orange (AO)/ethidium bromide (EB) staining, and Western blot assay were conducted to evaluate the drugs' effects in the cell clones.

Results: The cell clones expressing the D1 protein in MCF7 and MB231 cells result in distinct effects on the responses to chemotherapeutic treatments. Particularly with Gemzar, ectopic expression of cyclinD1 protein in MCF7 cells results in a potentiated effect, which is CDK4 kinase activity dependent, whereas in MB231 cells, an opposite effect was observed. Moreover, our results suggested that the distinct chemosensitivities among those cell clones were not resulted from accelerated cell cycle, cell proliferation driven by the cyclinD1CDK4/6-Rb-E2F signaling chain, rather, they were results of the cell cycle-independent functions led by cyclinD1 alone or in complex with CDK4.

Conclusions: Our results suggest that the functions of cyclinD1 protein in modulating chemoresponses in the MCF7 and MB231 cells are independent to its function as cell cycle initiator through activation of CDK4/6. Furthermore, the signals modulated by cyclinD1 upon treatment are determined by the drug and the cellular network.

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CyclinD1蛋白在MCF7和MDA-MB231细胞的化学反应调控中发挥不同的作用。

背景:CyclinD1是细胞周期起始和进展的重要传感器和激活因子;cyclinD1的过度表达与包括乳腺癌在内的多种人类癌症有关。在某些类型的癌症中，cyclinD1的升高被认为与肿瘤进展和对全身治疗的反应有关。目的:在这项研究中，我们期望解决人类乳腺癌的问题;cyclinD1在介导化学反应中的作用;以及协同cyclinD1干扰药物功能的信号通路。材料和方法:利用细胞克隆，在MCF7和MDA-MB231 (MB231)乳腺癌细胞中同时异位表达野生型或k112e突变的人cyclinD1蛋白，研究cyclinD1在化疗应答中的功能。本研究采用顺铂(CDDP)、5-氟尿嘧啶(5-FU)、Gemzar 3种药物;采用3-(4,5-二甲基噻唑-2-酰基)- 2,5 -二苯基溴化四唑(MTT)试验、细胞周期和细胞死亡分析、克隆存活试验、吖啶橙(AO)/溴化乙啶(EB)染色、Western blot等方法评价药物对细胞克隆的影响。结果:MCF7和MB231细胞中表达D1蛋白的细胞克隆对化疗反应有明显的影响。特别是在Gemzar中，MCF7细胞中cyclinD1蛋白的异位表达导致增强效应，这是CDK4激酶活性依赖的，而在MB231细胞中，观察到相反的效果。此外，我们的研究结果表明，这些细胞克隆之间不同的化学敏感性不是由cyclinD1 1cdk4 /6- rb - e2f信号链驱动的细胞周期加速和细胞增殖引起的，而是由cyclinD1单独或与CDK4复合导致的细胞周期独立功能的结果。结论:我们的研究结果表明，cyclinD1蛋白在MCF7和MB231细胞中调节化学反应的功能独立于其通过激活CDK4/6作为细胞周期启动器的功能。此外，cyclinD1在治疗过程中调节的信号是由药物和细胞网络决定的。

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

Journal of Carcinogenesis Environmental Science-Health, Toxicology and Mutagenesis

CiteScore

7.50

自引率

0.00%

发文量

审稿时长

15 weeks

期刊介绍： Journal of Carcinogenesis considers manuscripts in many areas of carcinogenesis and Chemoprevention. Primary areas of interest to the journal include: physical and chemical carcinogenesis and mutagenesis; processes influencing or modulating carcinogenesis, such as DNA repair; genetics, nutrition, and metabolism of carcinogens; the mechanism of action of carcinogens and modulating agents; epidemiological studies; and, the formation, detection, identification, and quantification of environmental carcinogens. Manuscripts that contribute to the understanding of cancer prevention are especially encouraged for submission