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A novel circular invasion assay mimics in vivo invasive behavior of cancer cell lines and distinguishes single-cell motility in vitro

机译:一种新型的圆形侵袭测定法模拟癌细胞系的体内侵袭行为,并在体外区分单细胞运动

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Background Classical in vitro wound-healing assays and other techniques designed to study cell migration and invasion have been used for many years to elucidate the various mechanisms associated with metastasis. However, many of these methods are limited in their ability to achieve reproducible, quantitative results that translate well in vivo . Such techniques are also commonly unable to elucidate single-cell motility mechanisms, an important factor to be considered when studying dissemination. Therefore, we developed and applied a novel in vitro circular invasion assay (CIA) in order to bridge the translational gap between in vitro and in vivo findings, and to distinguish between different modes of invasion. Method Our method is a modified version of a standard circular wound-healing assay with an added matrix barrier component (Matrigel?), which better mimics those physiological conditions present in vivo . We examined 3 cancer cell lines (MCF-7, SCOV-3, and MDA-MB-231), each with a different established degree of aggressiveness, to test our assay's ability to detect diverse levels of invasiveness. Percent wound closure (or invasion) was measured using time-lapse microscopy and advanced image analysis techniques. We also applied the CIA technique to DLD-1 cells in the presence of lysophosphatidic acid (LPA), a bioactive lipid that was recently shown to stimulate cancer cell colony dispersal into single migratory cells, in order to validate our method's ability to detect collective and individual motility. Results CIA method was found to be highly reproducible, with negligible levels of variance measured. It successfully detected the anticipated low, moderate, and high levels of invasion that correspond to in vivo findings for cell lines tested. It also captured that DLD-1 cells exhibit individual migration upon LPA stimulation, and collective behavior in its absence. Conclusion Given its ability to both determine pseudo-realistic invasive cell behavior in vitro and capture subtle differences in cell motility, we propose that our CIA method may shed some light on the cellular mechanisms underlying cancer invasion and deserves inclusion in further studies. The broad implication of this work is the development of a reproducible, quantifiable, high-resolution method that can be applied to various models, to include an unlimited number of parameters and/or agents that may influence invasion.
机译:背景技术设计用于研究细胞迁移和侵袭的经典体外伤口愈合测定法和其他技术已被使用多年,以阐明与转移相关的各种机制。然而,这些方法中的许多方法在获得可在体内良好翻译的可再现,定量结果的能力方面受到限制。这种技术通常也无法阐明单细胞运动机制,这是研究传播时要考虑的重要因素。因此,我们开发并应用了一种新型的体外循环侵袭测定法(CIA),以弥合体外和体内发现之间的翻译差距,并区分不同的侵袭模式。方法我们的方法是标准圆形伤口愈合分析的改良版,增加了基质屏障成分(Matrigel?),可更好地模拟体内存在的生理状况。我们检查了3种癌细胞系(MCF-7,SCOV-3和MDA-MB-231),每种具有不同的确定的侵袭程度,以测试我们的检测异种侵袭水平的能力。使用延时显微镜和先进的图像分析技术测量伤口闭合(或浸润)的百分比。我们还将CIA技术应用于溶血磷脂酸(LPA)存在的DLD-1细胞,溶血磷脂酸(LPA)是一种生物活性脂质,最近被证明可以刺激癌细胞集落分散到单个迁移细胞中,以验证我们的方法检测集体和非正常细胞的能力。个人运动。结果发现CIA方法具有很高的重现性,所测量的方差水平可忽略不计。它成功地检测到预期的低,中和高水平的浸润,与被测细胞系的体内发现相对应。它还捕获到DLD-1细胞在LPA刺激下表现出个体迁移,在LPA-1不存在时表现出集体行为。结论鉴于其能够在体外确定拟真侵袭性细胞行为并捕获细胞运动的细微差异,我们建议我们的CIA方法可能为癌症侵袭的细胞机制提供一些启示,值得进一步研究。这项工作的广泛含义是开发了一种可重现,可量化,高分辨率的方法,该方法可应用于各种模型,以包括可能影响入侵的无限数量的参数和/或代理。

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