Department of Life, Health and Environmental Sciences, University of L'Aquila, 67100 L'Aquila, Italy.
Pathology Unit, San Salvatore Hospital, Via Lorenzo Natali, 1, Coppito, 67100 L'Aquila, Italy.
Int J Mol Sci. 2022 Oct 4;23(19):11782. doi: 10.3390/ijms231911782.
The role of extracellular vesicles (EVs) as mediators of cell-to-cell communication in cancer progression is widely recognized. In vitro studies are routinely performed on 2D culture models, but recent studies suggest that 3D cultures could represent a more valid model. Human ovarian cancer cells CABA I were cultured by the hanging drop method to form tumor spheroids, that were moved to low adhesion supports to observe their morphology by Scanning Electron Microscopy (SEM) and to isolate the EVs. EVs release was verified by SEM and their identity confirmed by morphology (Transmission Electron Microscopy, TEM), size distribution (Nanoparticles Tracking Analysis), and markers (CD63, CD9, TSG-101, Calnexin). CABA I form spheroids with a clinically relevant size, above 400 μm; they release EVs on their external surface and also trap "inner" EVs. They also produce vasculogenic mimicry-like tubules, that bulge from the spheroid and are composed of a hollow lumen delimited by tumor cells. CABA I can be grown as multicellular spheroids to easily isolate EVs. The presence of features typical of in vivo tumors (inner entrapped EVs and vasculogenic mimicry) suggests their use as faithful experimental models to screen therapeutic drugs targeting these pro-tumorigenic processes.
细胞外囊泡 (EVs) 在癌症进展中作为细胞间通讯的介质的作用已被广泛认可。体外研究通常在 2D 培养模型上进行,但最近的研究表明 3D 培养可能更能代表真实情况。用人卵巢癌细胞 CABA I 通过悬滴法培养形成肿瘤球体,然后将其转移到低粘附支持物上,通过扫描电子显微镜 (SEM) 观察其形态,并分离 EVs。通过 SEM 验证 EVs 的释放,并通过形态学 (透射电子显微镜,TEM)、大小分布 (纳米颗粒跟踪分析) 和标志物 (CD63、CD9、TSG-101、Calnexin) 确认其身份。CABA I 形成具有临床相关大小(超过 400μm)的球体;它们在外部表面释放 EVs,也捕获“内部”EVs。它们还产生血管生成拟态样小管,从球体凸起,由肿瘤细胞限定的中空腔组成。CABA I 可以作为多细胞球体生长,便于分离 EVs。存在与体内肿瘤特征相似的特征(内部包裹的 EVs 和血管生成拟态)表明它们可用作筛选针对这些促肿瘤发生过程的治疗药物的忠实实验模型。
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