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首页> 外文期刊>Acta Obstetricia et Gynecologica Scandinavica: Official Publication of the Nordisk Forening for Obstetrik och Gynekologi >γ‐Secretase inhibition affects viability, apoptosis, and the stem cell phenotype of endometriotic cells
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γ‐Secretase inhibition affects viability, apoptosis, and the stem cell phenotype of endometriotic cells

机译:γ-分泌酶抑制会影响子宫内膜异位细胞的活力,细胞凋亡和干细胞表型

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Abstract Introduction Stem cells mediate cyclic regeneration of the endometrium. The upregulated expression of receptors and modulators of the notch signaling pathway in endometriosis suggests an involvement in the pathogenetic process. Here, we investigated the effects of notch pathway inhibition by a γ‐secretase inhibitor ( GSI ) on stemness‐associated properties of the epithelial endometriotic cell line 12Z and of primary endometriotic stroma cells. Material and methods 12Z cells and primary endometriotic stroma cells of 7 patients were treated with or without GSI , and analyzed for changes in gene expression by TaqMan low‐density arrays, quantitative PCR , and flow cytometry. The functional impact of GSI treatment was studied by MTT assay, cell cycle analysis, colony formation assay, annexin V apoptosis assay, and aldehyde dehydrogenase activity assays. Results In 12Z cells, GSI treatment reduced aldehyde dehydrogenase activity and colony formation, and induced a shift to the G2/M phase of the cell cycle. Cell viability was decreased and apoptosis was increased in both cell models. GSI further induced transcriptional downregulation of the stemness‐associated factors leukemia inhibitory factor receptor ( LIFR ), sex‐determining region Y (SRY)‐ box 2, interferon‐induced transmembrane protein 1, and hes‐related family bHLH transcription factor with YRPW motif 1, in 12Z cells and in primary cell cultures. Downregulation of LIFR expression by GSI was confirmed at the protein level by flow cytometry. Conclusions Our in vitro data suggest that application of GSI may be a worthwhile approach in the treatment of endometriosis that warrants further investigation.
机译:摘要引言干细胞介导子宫内膜的环状再生。在子宫内膜异位症中陷波信号通路的受体和调节剂的上调表达表明致病过程中的参与。在此,我们研究了γ-分泌酶抑制剂(GSI)对上皮内膜异位细胞系12Z和初级内膜异构体基质细胞的茎相关性质对γ-分泌酶抑制剂(GSI)的影响。材料和方法12Z细胞和7例患者的初级内膜体状细胞和没有GSI治疗,并分析Taqman低密度阵列,定量PCR和流式细胞术的基因表达的变化。通过MTT测定,细胞循环分析,菌落形成测定,膜蛋白V凋亡酶活性和醛脱氢酶活性测定来研究GSI处理的功能影响。结果12Z细胞,GSI治疗降低醛脱氢酶活性和菌落形成,并诱导细胞周期的G2 / M相移。细胞活力降低,两种细胞模型中的细胞凋亡增加。 GSI进一步诱导了茎干相关因子白血病抑制因子受体(LIFR),性别测定区域Y(Sry) - 盒2,干扰素诱导的跨膜蛋白1和HES相关的族BHLH转录因子与YRPW主题1的转录下调,在12z细胞和原代细胞培养物中。通过流式细胞术管在蛋白质水平处确认GSI的LIFR表达的下调。结论我们的体外数据表明,GSI的应用可能是治疗子宫内膜异位症的有价值的方法,要求进一步调查。

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