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通过定量相成像对休眠和活跃的人类癌细胞进行表征。

Characterization of dormant and active human cancer cells by quantitative phase imaging.

作者信息

Guo Peng, Huang Jing, Moses Marsha A

机构信息

Vascular Biology Program, Boston Children's Hospital, 300 Longwood Avenue, Boston, Massachusetts, 02115.

Department of Surgery, Harvard Medical School and Boston Children's Hospital, 300 Longwood Avenue, Boston, Massachusetts, 02115.

出版信息

Cytometry A. 2017 May;91(5):424-432. doi: 10.1002/cyto.a.23083. Epub 2017 Mar 17.

Abstract

The switch of tumor cells from a dormant, non-angiogenic phenotype to an active, angiogenic phenotype is a critical step in early cancer progression. To date, relatively little is known about the cellular behaviors of angiogenic and non-angiogenic tumor cell phenotypes. In this study, holographic imaging cytometry, a quantitative phase imaging (QPI) technique was used to continuously and non-invasively analyze, quantify, and compare a panel of fundamental cellular behaviors of angiogenic and non-angiogenic human osteosarcoma cells (KHOS) in a simple and economical way. Results revealed that angiogenic KHOS cells (KHOS-A) have significantly higher cell motility speeds than their non-angiogenic counterpart (KHOS-N) while no difference in their cell proliferation rates and cell cycle lengths were observed. KHOS-A cells were also found to have significantly smaller cell areas and greater cell optical thicknesses when compared with the non-angiogenic KHOS-N cells. No difference in average cell volumes was observed. These studies demonstrate that the morphology and behavior of angiogenic and non-angiogenic cells can be continuously, efficiently, and non-invasively monitored using a simple, quantitative, and economical system that does not require tedious and time-consuming assays to provide useful information about tumor dormancy. © 2017 International Society for Advancement of Cytometry.

摘要

肿瘤细胞从休眠的、非血管生成表型转变为活跃的、血管生成表型是癌症早期进展中的关键步骤。迄今为止,对于血管生成性和非血管生成性肿瘤细胞表型的细胞行为了解相对较少。在本研究中,使用全息成像细胞术这一定量相成像(QPI)技术,以简单且经济的方式对血管生成性和非血管生成性人骨肉瘤细胞(KHOS)的一组基本细胞行为进行连续、非侵入性的分析、量化和比较。结果显示,血管生成性KHOS细胞(KHOS-A)的细胞运动速度显著高于其非血管生成性对应细胞(KHOS-N),而在细胞增殖速率和细胞周期长度方面未观察到差异。与非血管生成性KHOS-N细胞相比,还发现KHOS-A细胞的细胞面积显著更小,细胞光学厚度更大。未观察到平均细胞体积有差异。这些研究表明,使用一个简单、定量且经济的系统,可以连续、高效且非侵入性地监测血管生成性和非血管生成性细胞的形态和行为,该系统无需繁琐且耗时的检测就能提供有关肿瘤休眠的有用信息。© 2017国际细胞计量学促进协会。

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