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Distinct effects of epirubicin cisplatin and cyclophosphamide on ovarian somatic cells of prepuberal ovaries

机译:表柔比星顺铂和环磷酰胺对青春期前卵巢体细胞的不同作用

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摘要

culture models were used to characterize the effects of chemotherapeutic drugs and of LH on somatic cells from prepuberal mouse ovaries. All cell types (pre- and granulosa cells, pre-thecal and OSE cells) underwent apoptosis following Epirubicin (0.5μM) exposure for 24hrs (about 60%) and 48hrs (>80%). Cisplatin (10μM) and the Cyclophosphamide active metabolite, Phosphoramide Mustard (10μM), didn’t cause apoptosis in 90% of pre-thecal and pre-granulosa cells up to 72hrs of exposure, although they suffered extensive DNA damage and cell cycle arrest, and acquired stress induced premature senescence (SIPS) features. Cultured granulosa cells didn’t show evident DNA damage and remained viable without acquiring SIPS features; OSE cells were resistant to apoptosis and SIPS but not to DNA damage. These latter, like pre-thecal and pre-granulosa cells, were able of efficient DNA repair involving MLH1-dependent MMR pathways. SIPS features were also observed in ovary after treatment with Cisplatin. LH (200mIU/mL) didn’t significantly influence apoptosis, SIPS and DNA damage but favoured DNA repair. These results show that somatic cells of prepuberal ovary response to drugs in different ways, either undergoing apoptosis or SIPS, either showing resistance to Cisplatin and Phosphoramide Mustard. Moreover, a new role of LH in promoting DNA repair was shown.
机译:培养模型用于表征化学治疗药物和LH对来自青春期前小鼠卵巢的体细胞的影响。在表柔比星(0.5μM)暴露24小时(约60%)和48小时(> 80%)后,所有细胞类型(前和颗粒细胞,鞘前和OSE细胞)均发生凋亡。顺铂(10μM)和环磷酰胺活性代谢产物磷酰胺芥末(10μM)直到暴露72小时后,仍未引起90%的鞘前和颗粒前细胞凋亡,尽管它们遭受了广泛的DNA损伤和细胞周期停滞,以及获得性应激诱发的早衰(SIPS)功能。培养的颗粒细胞没有显示出明显的DNA损伤,并且在没有获得SIPS功能的情况下仍然可以存活。 OSE细胞对细胞凋亡和SIPS具有抵抗力,但对DNA损伤没有抵抗力。这些后者,像鞘前和颗粒前细胞一样,能够进行有效的DNA修复,涉及依赖MLH1的MMR途径。顺铂治疗后在卵巢中也观察到了SIPS特征。 LH(200mIU / mL)不会明显影响细胞凋亡,SIPS和DNA损伤,但有利于DNA修复。这些结果表明,青春期前的体细胞对药物的反应不同,无论是经历凋亡还是SIPS,都表现出对顺铂和磷酰胺芥菜的抗性。而且,显示了LH在促进DNA修复中的新作用。

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