首页> 外文期刊>Clinical neurology and neurosurgery >Medroxyprogesterone effects on colony growth, autophagy and mitochondria of C6 glioma cells are augmented with tibolone and temozolomide Cell kinetic and electron microscopical studies with a broad review of the literature
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Medroxyprogesterone effects on colony growth, autophagy and mitochondria of C6 glioma cells are augmented with tibolone and temozolomide Cell kinetic and electron microscopical studies with a broad review of the literature

机译:C6胶质瘤细胞的殖民地生长,自噬和线粒体的菌丝生长,自噬和线粒体的影响因紫龙和替替莫唑胺细胞动力学和电子显微镜研究而言,具有广泛的审查文献

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Objective: Risk of high grade gliomas is lower in young females and its incidence enhances after menopause suggesting likely protective roles of female hormones. Hormone replacement therapy (HRT) was widely employed to treat osteoporosis and some epidemiological studies showed that HRT regimes including progesterone analogs such as medroxyprogesterone acetate (MPA) decreased risk of glial tumors. Tibolone is a unique progesterone analog employed in HRT with tissue specific estrogenic effects and stimulates gene expressions very similar to those induced by MPA. Tibolone's pro-estrogenic effects occur particularly in bone and brain and both MPA and tibolone inhibit AKR1C enzymes, which involve in temozolomide chemoresistance. Hence, we aimed to investigate interactions between MPA, tibolone and temozolomide in modification of glioma cell growth and fine structure. Patients and Methods: For our studies, we have particularly chosen C6 rat glioma cell line due to several reasons: i) We previously showed that MPA reduced growth and induced procarbazine-sensitization in C6 cells; ii) temozolomide has a triazene-type molecular structure like procarbazine; iii) other groups previously showed that C6 glioma cell line is more resistant to temozolomide than human glioma cells; hence it may provide a native model of chemoresistance. Monolayer plating efficacy, soft agar colony growth, 3D-spheroid S-phase (as determined by BrdU-labeling) and electron microscopical analyses were performed to assess mutual interactions between MPA, tibolone and temozolomide. Results: MPA inhibited clonogenic growth of C6 glioma and this effect is augmented by both tibolone and temozolomide. MPA and tibolone inhibited DNA synthesis in C6 glioma spheroids to similar levels which can be achieved with temozolomide. Electron microscopical analyses revealed synergisms between MPA, tibolone and temozolomide involved mitochondria! proliferation, condensation, mitophagy and autophagy. Conclusions: MPA and tibolone shall be studied in further experimental models of glioblastoma in vitro and in vivo.
机译:目的:年轻女性高级胶质瘤的风险较低,其发生耐药性在绝经后提高雌性激素的保护作用。激素替代疗法(HRT)被广泛用于治疗骨质疏松症,一些流行病学研究表明,包括孕酮类似物,如MEGROXYPRAGENTONE(MPA)的HRT制度降低了胶质肿瘤的风险。 Tibolone是一种在HRT中使用的孕酮类似物,具有组织特异性雌激素作用,并刺激与MPA诱导的那些非常相似的基因表达。 Tibolone的促培养作用特别是在骨骼和脑和脑中,MPA和Tibolone抑制AKR1C酶,其涉及替替莫唑胺化学性。因此,我们旨在研究MPA,紫红素和替替唑胺类酰胺在胶质瘤细胞生长和细结构的改性中的相互作用。患者和方法:对于我们的研究,我们特别选择的C6大鼠胶质瘤细胞系引起的几个原因:i)我们之前表明MPa降低了C6细胞中的生长和诱导的ProCarbazine致敏; ii)替替唑胺具有三缩型分子结构,如ProCarbazine; III)其他群体以前表明C6胶质瘤细胞系比人胶瘤细胞更耐药;因此,它可以提供化学化的本地模型。单层电镀功效,软琼脂菌落生长,3D-球形S相(如Brdu标记测定)和电子显微镜分析,以评估MPa,紫红素和替莫唑胺之间的相互作用。结果:MPA抑制C6胶质瘤的克隆菌生长,并且通过紫红素和替替莫唑胺增强这种效果。 MPA和Tibolone在C6胶质瘤球体中抑制DNA合成,以通过替代唑烷二族来实现的类似水平。电子显微镜分析揭示了MPA,蒂尔酮和替替唑胺涉及线粒体的协同作用!增殖,缩合,含有型自噬。结论:MPA和TIBOLONE应在体外和体内进一步的胶质母细胞瘤的实验模型中进行研究。

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