Response in shape and size of individual p31 cancer cells to cisplatin and ouabain: a computerized image analysis of cell halo characteristics during continuous perfusion.

Cytometry Pub Date : 2000-07-01
P Behnam-Motlagh, K Grankvist, R Henriksson, K G Engström
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Abstract

Background: Volume regulation is essential for cellular functions, including cell death, such as apoptosis. Flow cytometry is standard for nonadherent cells, such as blood cells. Our aim was to explore image analysis methods to study adherent cancer cells of a solid tumor.

Methods: P31 mesothelioma cells were perifused (40 min) and studied by phase-contrast microscopy. A noise reduction of the cell contour was tested to more accurately yield the cell shape factor (SF). The optical halo around the cell was analyzed for information about membrane blebbing.

Results: The projected cell area (PCA) slowly increased under control perfusion, the halo outside more than the halo inside. Cisplatin (apoptosis) caused an immediate increase in the PCA-halo outside (5.9 +/- 1.2 %, P < 0.01, 1-5 min) and the SF indicated decreased roundness (P < 0.05). The SF-halo inside became more irregular than the outside, which was different from the control cells. The morphology reflected instant blebbing, and the cell bodies showed fragmentation after about 20 min. Ouabain resulted in only small changes in PCA and SF, significantly different from both control and cisplatin conditions.

Conclusions: Image analysis (PCA and SF) on perifused adherent cancer cells may serve as a tool to follow the sensitivity of cancer chemotherapy and to study cell death patterns.

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单个p31癌细胞对顺铂和瓦巴因的形状和大小的反应:连续灌注期间细胞晕特征的计算机图像分析。
背景:体积调节对细胞功能至关重要,包括细胞死亡,如凋亡。流式细胞术是检测非贴壁细胞(如血细胞)的标准方法。我们的目的是探索图像分析方法来研究附着癌细胞的实体瘤。方法:P31间皮瘤细胞经周灌洗40 min,相衬显微镜观察。对细胞轮廓进行降噪测试,以更准确地产生细胞形状因子(SF)。通过分析细胞周围的光晕来获取膜泡的信息。结果:在控制灌注下,细胞投影面积(PCA)缓慢增加,外晕大于内晕。顺铂(细胞凋亡)可立即引起细胞外pca光晕增加(5.9 +/- 1.2%,P < 0.01, 1 ~ 5 min), SF圆度降低(P < 0.05)。内部的sf光晕比外部的更不规则,这与对照细胞不同。形态学表现为瞬间起泡,约20 min后细胞体出现碎裂。瓦巴因对PCA和SF的影响较小,与对照组和顺铂组均有显著差异。结论:对浸润的贴壁癌细胞的图像分析(PCA和SF)可作为跟踪肿瘤化疗敏感性和研究细胞死亡模式的工具。
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