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首页> 外文期刊>Oncology letters >Overexpression of sigma-1 receptor in MCF-7 cells enhances proliferation via the classic protein kinase C subtype signaling pathway
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Overexpression of sigma-1 receptor in MCF-7 cells enhances proliferation via the classic protein kinase C subtype signaling pathway

机译:MCF-7细胞中Sigma-1受体的过度表达通过经典蛋白激酶C亚型信号通路增强增殖

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摘要

Sigma-1 receptor (sigma-1R), a 25-kDa integral membrane protein, is expressed at a high density in various tumor cell lines and its ligands mediate tumor cell proliferation. However, the effect of this receptor on proliferation and the associated intracellular molecules in tumors remains unclear. The present study aimed to investigate the effect of sigma-1R overexpression on MCF-7 cell proliferation and the associated intracellular molecules that serve a key role in this process. The sigma-1R proliferative function was examined by comparing the proliferation rates of a sigma-1R-overexpressing line, MCF-41 with a sigma-1R-defective line, MCF-7, in culture media with various serum concentrations. The results demonstrated that MCF-41 cells grew significantly faster compared with MCF-7 cells, indicating a proliferation-enhancing receptor function. This proliferation-enhancing effect was completely eliminated by adding a PKC inhibitor to the culture media for MCF-41 cells. To identify which PKC subtype affects the proliferative function of sigma-1R, five inhibitors of PKC subtypes or enzymes involved in the PKC signaling cascade were introduced to MCF-7 and MCF-41 cell culture media and their effects on cell proliferation were compared. It was revealed that only the classic PKC subtype inhibitor, GF109203x, significantly inhibited MCF-41 cell proliferation compared with the MCF-7 line. In conclusion, among PKC iso-enzymes only classic PKC subtype enzymes serve an important role in sigma-1R overexpression enhancing MCF-7 cell proliferation.
机译:Sigma-1受体(Sigma-1R),25-KDA整体膜蛋白,在各种肿瘤细胞系中以高密度表达,其配体介导肿瘤细胞增殖。然而,该受体对肿瘤中的增殖和相关细胞内分子的影响仍然不清楚。本研究旨在探讨Sigma-1R过表达对MCF-7细胞增殖的影响和在该过程中发挥关键作用的相关细胞内分子。通过将Sigma-1R过表达线,MCF-41与Sigma-1R缺陷的线,MCF-7在具有各种血清浓度的培养基中的培养培养基中的培养培养基,检查Sigma-1R增殖函数。结果表明,与MCF-7细胞相比,MCF-41细胞增长显着更快,表明增强增强受体功能。通过向MCF-41细胞添加PKC抑制剂来完全消除这种增强效果。为了确定哪种PKC亚型影响Sigma-1R的增殖函数,将参与PKC信号传导级联的PKC亚型或酶的五种抑制剂引入MCF-7和MCF-41细胞培养基及其对细胞增殖的影响。据揭示,与MCF-7线相比,只有经典的PKC亚型抑制剂,GF109203x显着抑制MCF-41细胞增殖。总之,在PKC ISO-酶中,经典PKC亚型酶在Sigma-1R过表达中提供重要作用,增强MCF-7细胞增殖。

著录项

  • 来源
    《Oncology letters》 |2018年第2期|共7页
  • 作者单位

    China Jiliang Univ Coll Life Sci Dept Pharm 258 Xueyan St Hangzhou 310018 Zhejiang Peoples R;

    China Jiliang Univ Coll Life Sci Dept Pharm 258 Xueyan St Hangzhou 310018 Zhejiang Peoples R;

    China Jiliang Univ Coll Life Sci Dept Pharm 258 Xueyan St Hangzhou 310018 Zhejiang Peoples R;

    China Jiliang Univ Coll Life Sci Dept Pharm 258 Xueyan St Hangzhou 310018 Zhejiang Peoples R;

    China Jiliang Univ Coll Life Sci Dept Pharm 258 Xueyan St Hangzhou 310018 Zhejiang Peoples R;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学;
  • 关键词

    sigma-1 receptor; protein kinase C; MCF-7; overexpression; proliferation;

    机译:Sigma-1受体;蛋白激酶C;MCF-7;过表达;增殖;

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