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Single and Combinational siRNA Therapy of Cancer Cells: Probing Changes in Targeted and Nontargeted Mediators after siRNA Treatment

机译:癌细胞的单一和联合siRNA治疗:在siRNA治疗后探索靶向和非靶向介体的变化

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摘要

Cancer cells are known to be heterogeneous and plastic, which imparts innate and acquired abilities to resist molecular targeting by short interfering RNA (siRNA). Not all cancer cells in a population would show a similar responsiveness to targeting of genes critical for their survival and even the responders could quickly transform and switch to alternative mechanism(s) for their survival. This study was designed to look at this phenomenon by analyzing the effect of siRNA silencing of selected protein mRNAs involved in cell survival and proliferation on other protein mRNAs that could contribute to cell survival. We compared the gene expression profile of the initial population after siRNA silencing to the subpopulation that survived the siRNA silencing, to identify potential overexpressions that might explain the cell survival. Our studies show that silencing well-selected protein mRNAs simultaneously could offer advantages compared to individual siRNA silencing due to an additional impact on the expression level of certain protein mRNAs. We also demonstrate that overexpression of certain protein mRNAs could explain the innate unresponsiveness of a subpopulation of cells. These observations could be a stepping stone for further investigation of the possibility of significant synergistic effect for this combinational RNA interference strategy.
机译:众所周知,癌细胞是异质的和可塑性的,可通过短干扰RNA(siRNA)赋予抵抗分子靶向的先天和后天能力。并非群体中的所有癌细胞都会对针对其生存至关重要的基因表现出相似的反应性,甚至响应者也可以迅速转化并转换为生存的其他机制。本研究旨在通过分析参与细胞存活和增殖的选定蛋白质mRNA的siRNA沉默对可能有助于细胞存活的其他蛋白质mRNA的影响来研究这种现象。我们将siRNA沉默后的初始种群的基因表达谱与siRNA沉默后的亚群进行了比较,以确定可能解释细胞存活的潜在过表达。我们的研究表明,与单独的siRNA沉默相比,同时沉默选择良好的蛋白质mRNA可能会提供优势,因为这会对某些蛋白质mRNA的表达水平产生额外影响。我们还证明了某些蛋白质mRNA的过表达可以解释细胞亚群的先天无反应性。这些观察结果可能是进一步研究这种组合RNA干扰策略产生显着协同效应的可能性的垫脚石。

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