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Metastasis-associated mts1 gene expression is down-regulated by heat shock in variant cell lines of the B16 murine melanoma

机译:转移相关的 mts1 基因表达因 B16 小鼠黑色素瘤变异细胞系中的热休克而下调

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Tumour cells are more heat sensitive than corresponding normal cells but the reasons for this are poorly understood. Here we report that induction of heat shock proteins was associated with a down-regulation of the metastasis associatedmts1 gene in BL6-B16 murine melanoma cells, and the heat-resistant HTG variant of the BL6 line. Melanocyte stimulating hormone, which does not affect B16 cell proliferation but upregulatesmts1 expression, only marginally enhanced heat shock protein expression in F1 cells as determined by immunohistochemical methods. Retinoic acid, which inhibits cell proliferation and down-regulates themts1 gene, reduced heat shock protein expression in the ML8-B16 variant line. This suggests that the changes in the heat shock protein expression reported here may be cell proliferation related. Heat shock proteins are known to stabilize microtubules, whereasmts1 has been implicated in their depolymerization. Taxol, which stabilizes microtubules and arrests cells at the G1phase of the cell cycle, down-regulatedmts1 gene expression in both F1 and ML8 lines. Taxol also reduced heat shock protein expression in ML8 cells. These data suggest opposing functions of heat shock proteins and themts1 gene in microtubule polymerization, and may provide a rationale for the use of hyperthermia as a treatment for tumours
机译:肿瘤细胞比相应的正常细胞更热敏,但其原因知之甚少。在这里,我们报告了热休克蛋白的诱导与 BL6-B16 小鼠黑色素瘤细胞中转移相关 mts1 基因的下调以及 BL6 系的耐热 HTG 变体有关。黑色素细胞刺激素不影响 B16 细胞增殖但上调 mts1 表达,仅略微增强 F1 细胞中热休克蛋白的表达,如免疫组织化学方法测定的那样。维甲酸可抑制细胞增殖并下调 themts1 基因,降低 ML8-B16 变异系中热休克蛋白的表达。这表明这里报道的热休克蛋白表达的变化可能与细胞增殖有关。已知热休克蛋白可以稳定微管,而 mts1 与它们的解聚有关。紫杉醇可稳定微管并在细胞周期的 G1 期阻滞细胞,下调 F1 和 ML8 系中 mts1 基因的表达。紫杉醇还降低了ML8细胞中热休克蛋白的表达。这些数据表明热休克蛋白和 themts1 基因在微管聚合中的相反功能,并可能为使用热疗治疗肿瘤提供理由

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