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首页> 外文期刊>International journal of molecular medicine >Long non?coding RNA FOXD2?AS1 regulates the?tumorigenesis and progression of breast cancer via the S100 calcium binding protein A1/Hippo signaling pathway
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Long non?coding RNA FOXD2?AS1 regulates the?tumorigenesis and progression of breast cancer via the S100 calcium binding protein A1/Hippo signaling pathway

机译:长的非?编码RNA FOXD2?AS1通过S100钙结合蛋白A1 / Hippo信号通路调节肿瘤瘤和乳腺癌的进展

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Breast cancer is one of the most prevalent cancer types and is accompanied by a high incidence and mortality rate, severely threatening women's health globally. Long non?coding RNA forkhead box D2 adjacent apposite strand RNA 1 (lncRNA FOXD2?AS1) has been identified to function as an oncogene in human cancers; however, it has rarely been investigated in breast cancer. The aim of the present study was to investigate the role of FOXD2?AS1 in breast cancer, and to clarify the underlying mechanisms. The expression of FOXD2?AS1 in breast cancer cell lines was first quantified by reverse transcription?quantitative PCR, and the biological function of FOXD2?AS1 was then determined. Cellular proliferative ability was determined by Cell Counting kit?8 assay, and wound healing and Transwell assays were conducted to assess the cell migratory and invasive ability. Corresponding protein expression levels were determined by western blot analysis. In addition, experimental animal models were established by the subcutaneous injection of MDA?MB?468 cells into the right axillary lymph nodes of BALB/c nude mice, and the effects of FOXD2?AS1 on tumor growth were observed. The results indicated that FOXD2?AS1 expression was upregulated in breast cancer cell lines, and that FOXD2?AS1 downregulation significantly inhibited the proliferation, migration and invasiveness of MCF?7 and MDA?MB?468 cells. S100 calcium binding protein A1 (S100A1) was also upregulated in breast cancer cell lines and was positively regulated by FOXD2?AS1. Furthermore, the inhibition of S100A1 and the overexpression of the serine/threonine?protein kinase, large tumor suppressor homolog 1 (LATS1), inhibited the FOXD2?AS1?induced cellular proliferation, migration and invasiveness in breast cancer. Experimental mouse models revealed that FOXD2?AS1 downregulation significantly inhibited tumor growth, and that the levels of phosphorylated (p?)YAP and p?LATS1 were upregulated by FOXD2?AS1 knockdown, indicating that the inhibition of FOXD2?AS1 activated Hippo/yes?associated protein signaling. On the whole, the findings of the present study suggest that the FOXD2?AS1/S100A1/Hippo axis is involved in the tumorigenesis and progression of breast cancer. In the future, these may contribution to the identification of more effective breast cancer treatments.
机译:乳腺癌是最普遍的癌症类型之一,伴随着高发病率和死亡率,严重威胁到全球妇女的健康状况。长的非α编码RNA尖头箱D2相邻的己二维RNA 1(LNCRNA FOXD2β-AS1)已经鉴定为用作人类癌症中的癌基因;然而,它很少在乳腺癌中进行研究。本研究的目的是探讨Foxd2吗?As1在乳腺癌中的作用,并阐明潜在机制。通过逆转录α定量P​​CR,首先使FoxD2的表达式是乳腺癌细胞系中的表达,然后测定Foxd2的生物学功能。细胞增殖能力通过细胞计数试剂盒α测定,进行伤口愈合和转发测定以评估细胞迁移和侵袭能力。通过蛋白质印迹分析测定相应的蛋白质表达水平。此外,通过皮下注射MDA?MBαmBβ268细胞建立了实验动物模型,进入BALB / C裸鼠的右腋窝淋巴结,观察到FOXD2的效果对肿瘤生长。结果表明,乳腺癌细胞系中的福索达德2表达,并且Foxd2?As1下调显着抑制MCF?7和MB?MB?468细胞的增殖,迁移和侵袭性。 S100钙结合蛋白A1(S100A1)也在乳腺癌细胞系中上调,并通过Foxd2呈正调节αsa1。此外,S100A1的抑制和丝氨酸/苏氨酸的过表达?蛋白激酶,大型肿瘤抑制同源1(LATS1)抑制FoxD2?As1?诱导乳腺癌的细胞增殖,迁移和侵袭性。实验小鼠模型显示Foxd2?AS1下调显着抑制肿瘤生长,并且通过Foxd2敲低来上调磷酸化(P?)yap和p?Lats1的水平,表明FoxD2的抑制率为Hippo /是?相关蛋白质信号。总的来说,本研究的发现表明FOXD2?AS1 / S100A1 /河马轴涉及肿瘤癌的肿瘤鉴定和进展。在未来,这些可能对鉴定更有效的乳腺癌治疗来贡献。

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