首页> 外文期刊>Endocrine-related cancer >miR-200c is aberrantly expressed in leiomyomas in an ethnic-dependent manner and targets ZEBs, VEGFA, TIMP2, and FBLN5
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miR-200c is aberrantly expressed in leiomyomas in an ethnic-dependent manner and targets ZEBs, VEGFA, TIMP2, and FBLN5

机译:miR-200c以依赖种族的方式在平滑肌瘤中异常表达,并靶向ZEB,VEGFA,TIMP2和FBLN5

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MicroRNA-200c (miR-200c) through repression of specific target genes has been associated with cellular transition, tumorigenesis, and tissue fibrosis. We explored the expression and functional aspects of miR-200c in genesis of leiomyomas (LYO), benign uterine tumors with fibrotic characteristic. Using LYO and matched myometrium (MYO; n=76) from untreated and from patients exposed to hormonal therapies (GNRH agonist (GNRHa), Depo-Provera, and oral contraceptives), we found that miR-200c was expressed at significantly lower levels (P0.05) in LYO as compared with MYO. These levels were lower in LYO from African Americans as compared with Caucasians, patients experiencing abnormal uterine bleeding and those exposed to GNRHa therapy. Gain-of-function of miR-200c in isolated leiomyoma smooth muscle cells (LSMCs), myometrial smooth muscle cells (MSMCs), and leiomyosarcoma cell line (SKLM-S1) repressed ZEB1/ZEB2 mRNAs and proteins, with concurrent increase in E-cadherin (CDH1) and reduction in vimentin expression, phenotypic alteration, and inhibition of MSMC and LSMC proliferations. We further validated TIMP2, FBLN5, and VEGFA as direct targets of miR-200c through interaction with their respective 3′ UTRs, and other genes as determined by microarray analysis. At tissue levels, LYO expressed lower levels of TIMP2 and FBLN5 mRNAs but increased protein expressions, which to some extent altered due to hormonal exposure. Given the regulatory functions of ZEBs, VEGFA, FBLN5, and TIMP2 on cellular activities that promote cellular transition, angiogenesis, and matrix remodeling, we concluded that altered expression of miR-200c may have a significant impact on the outcome of LYO growth, maintenance of their mesenchymal and fibrotic characteristics, and possibly their associated symptoms.
机译:通过抑制特定靶基因的MicroRNA-200c(miR-200c)与细胞转化,肿瘤发生和组织纤维化有关。我们探讨了miR-200c在平滑肌瘤(LYO),具有纤维化特征的良性子宫肿瘤的发生中的表达和功能方面。使用未经治疗的LYO和匹配的子宫肌层(MYO; n = 76),以及未经激素治疗的患者(GNRH激动剂(GNRHa),Depo-Provera和口服避孕药),我们发现miR-200c的表达水平明显较低(与MYO相比,LYO中的P <0.05)。与白种人,患有异常子宫出血的患者和接受GNRHa治疗的患者相比,非洲裔美国人的LYO中这些水平较低。在分离的平滑肌瘤平滑肌细胞(LSMC),肌层平滑肌细胞(MSMC)和平滑肌肉瘤细胞系(SKLM-S1)中获得miR-200c的功能可抑制ZEB1 / ZEB2 mRNA和蛋白,同时增加E-钙粘蛋白(CDH1)和波形蛋白表达的减少,表型改变以及对MSMC和LSMC增殖的抑制作用。我们进一步通过与微阵列分析确定的TIMP2,FBLN5和VEGFA与其各自的3'UTR和其他基因的相互作用,验证了它们是miR-200c的直接靶标。在组织水平,LYO表达较低水平的TIMP2和FBLN5 mRNA,但蛋白质表达增加,这在一定程度上由于激素暴露而改变。鉴于ZEB,VEGFA,FBLN5和TIMP2对促进细胞迁移,血管生成和基质重塑的细胞活性的调节功能,我们得出结论,改变miR-200c的表达可能对LYO生长,维持和维持LYO的结果产生重大影响。它们的间质和纤维化特征,以及可能的相关症状。

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