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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >IR spectroscopy as a new tool for evidencing antitumor drug signatures.
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IR spectroscopy as a new tool for evidencing antitumor drug signatures.

机译:红外光谱法是证明抗肿瘤药物特征的新工具。

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There is a growing interest for screening antitumor drugs for their mechanism of action on cancer cells. Yet, screening for "modes of action" presents a technical challenge that is beyond the capability of conventional methods used in cellular or molecular biology. Several studies have highlighted the advantages of using infrared spectroscopy for diagnostic purposes at the clinical level for identifying cell types. In the present work, we suggest that the Fourier Transform Infrared (FTIR) spectrum of cells exposed to anti-cancer drugs could offer a unique opportunity to obtain a fingerprint of all molecules present in the cells and to observe, with a high sensitivity, the metabolic changes induced by potential anti-cancer drugs. Ouabain is one of the most potent cardenolides, which acts by inhibiting sodium pump activity. Cardenolides represent a class of compounds that are intended to soon enter clinical trials in oncology. In order to evaluate the potential of infrared spectroscopy to yield a signature for ouabain action on cancer cells, human prostate cancer PC-3 cells were treated with 36 nM ouabain, a sub-lethal concentration. Using ouabain as a model, we have thus demonstrated the possibility of using IR spectroscopy in the assessment of the global effects of an investigational compound on the cell constituents, thus contributing to setting up a new method for screening for novel anti-cancer agents in general, and potential anti-cancer cardenolides in particular. The most spectacular data obtained strongly suggest a modification in the nature of the cell lipids.
机译:对于筛选抗肿瘤药物对癌细胞的作用机理的兴趣日益增长。然而,“作用方式”的筛选提出了技术挑战,其超出了细胞或分子生物学中使用的常规方法的能力。多项研究强调了在临床水平上使用红外光谱法进行诊断以识别细胞类型的优势。在目前的工作中,我们建议暴露于抗癌药物的细胞的傅立叶变换红外(FTIR)光谱可以为获得细胞内存在的所有分子的指纹并以高灵敏度观察其分子结构提供独特的机会。由潜在的抗癌药物引起的代谢变化。瓦巴因是最有效的烯醇内酯之一,可通过抑制钠泵的活性发挥作用。胡萝卜素代表一类化合物,旨在很快进入肿瘤学临床试验。为了评估红外光谱法产生哇巴因作用于癌细胞的特征的潜力,将人前列腺癌PC-3细胞用亚致命浓度的36 nM哇巴因进行了处理。因此,以哇巴因为模型,我们已经证明了使用红外光谱法评估待研究化合物对细胞成分的整体作用的可能性,从而有助于建立一种新的筛选新型抗癌药物的方法。 ,尤其是潜在的抗癌心内酯。获得的最壮观的数据强烈暗示了细胞脂质性质的改变。

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