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内在和获得性顺铂耐药人黑色素瘤细胞系的分级:红外 ATR 研究。

Grading of intrinsic and acquired cisplatin-resistant human melanoma cell lines: an infrared ATR study.

机构信息

Department of Physics and the Cancer Research Center, Ben-Gurion University, Beer-Sheva 84105, Israel.

出版信息

Eur Biophys J. 2011 Jun;40(6):795-804. doi: 10.1007/s00249-011-0695-2. Epub 2011 Apr 7.

DOI:10.1007/s00249-011-0695-2
PMID:21472431
Abstract

Attenuated total reflection (ATR) spectroscopy is used as an in vitro optical approach for the diagnosis and characterization of cell and tissue pathology. In comparison with the more conventional FTIR microspectroscopy that relies on transmission of IR radiation, ATR spectroscopy uses the evanescent wave technique, which is a step forward toward in vivo research. The aim of the present investigation was to examine the potential of ATR spectroscopy to differentiate between drug-resistant and drug-sensitive melanoma cell lines. We studied two human melanoma parental cell lines, GA and BG, and their cisplatin-resistant counterparts, GAC and BGC, respectively, which were derived by survival selection with this anticancer drug. Cisplatin cytotoxicity was measured on the four cell lines, and their relative resistance to cisplatin was established: BGC > BG > GAC > GA. Different resistance mechanisms were noticed between the two parental groups in accordance with their spectrum. ATR spectra-based cluster analysis of the selective biomarkers, such as phosphate and RNA/DNA, were found useful in differentiating sensitive from resistant cells. Normalized and absolute values of the differences between spectra were employed to compare between the two parental groups. It was possible to predict the relative cisplatin resistance between the cell lines using the discriminant classifying function. The success rates in predicting cisplatin resistance in these cells was 88 and 81% for GA versus GAC and BG versus BGC, respectively. These results support the further development of the ATR technique as a simple, in vitro, reagent-free method to identify drug resistance in cancer cells.

摘要

衰减全反射(ATR)光谱学被用作体外光学方法,用于诊断和表征细胞和组织病理学。与更传统的依赖于红外辐射透射的 FTIR 微光谱学相比,ATR 光谱学使用消逝波技术,这是向体内研究迈进的一步。本研究的目的是探讨 ATR 光谱学区分耐药和敏感黑色素瘤细胞系的潜力。我们研究了两个人类黑色素瘤亲本细胞系 GA 和 BG,以及它们各自的顺铂耐药对应物 GAC 和 BGC,这些耐药对应物是通过用这种抗癌药物进行生存选择而衍生的。在这四个细胞系上测量了顺铂的细胞毒性,并确定了它们对顺铂的相对耐药性:BGC > BG > GAC > GA。根据它们的光谱,注意到两个亲本群体之间存在不同的耐药机制。基于 ATR 光谱的选择性生物标志物(如磷酸盐和 RNA/DNA)聚类分析,有助于区分敏感细胞和耐药细胞。使用归一化和光谱之间差异的绝对值来比较两个亲本群体。使用判别分类函数可以预测细胞系之间的相对顺铂耐药性。GA 与 GAC 和 BG 与 BGC 之间的顺铂耐药性预测成功率分别为 88%和 81%。这些结果支持进一步开发 ATR 技术作为一种简单、体外、无需试剂的方法,用于识别癌细胞中的药物耐药性。

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本文引用的文献

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Attenuated total reflectance spectroscopy: a promising technique for early detection of premalignancy.衰减全反射光谱学:一种有前途的癌前病变早期检测技术。
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IR spectroscopy reveals effect of non-cytotoxic doses of anti-tumour drug on cancer cells.红外光谱揭示了非细胞毒性剂量的抗癌药物对癌细胞的影响。
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Early detection of premalignant changes in cell cultures using light-induced fluorescence spectroscopy.利用光诱导荧光光谱法早期检测细胞培养物中的癌前病变。
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