Dentistry-Regenerative Biomaterials, Radboudumc, Nijmegen, The Netherlands.
Cell Prolif. 2024 Sep;57(9):e13693. doi: 10.1111/cpr.13693. Epub 2024 Jun 20.
Most bone metastases are caused by primary breast or prostate cancer cells settling in the bone microenvironment, affecting normal bone physiology and function and reducing 5-year survival rates to 10% and 6%, respectively. To expedite clinical availability of novel and effective bone metastases treatments, reliable and predictive in vitro models are urgently required to screen for novel therapies as current in vitro 2D planar mono-culture models do not accurately predict the clinical efficacy. We herein engineered a novel human in vitro 3D co-culture model based on spheroids to study dynamic cellular quantities of (breast or prostate) cancer cells and human bone marrow stromal cells and screen chemotherapeutic efficacy and specificity of the common anticancer drug cisplatin. Bone metastatic spheroids (BMSs) were formed rapidly within 24 h, while the morphology of breast versus prostate cancer BMS differed in terms of size and circularity upon prolonged culture periods. Prestaining cell types prior to BMS formation enabled confocal imaging and quantitative image analysis of in-spheroid cellular dynamics for up to 7 days of BMS culture. We found that cancer cells in BMS proliferated faster and were less susceptible to cisplatin treatment compared to 2D control cultures. Based on these findings and the versatility of our methodology, BMS represent a feasible 3D in vitro model for screening of new bone cancer metastases therapies.
大多数骨转移是由原发性乳腺癌或前列腺癌细胞在骨微环境中定居引起的,影响正常骨生理和功能,使 5 年生存率分别降至 10%和 6%。为了加速新型有效骨转移治疗方法的临床应用,迫切需要可靠和可预测的体外模型来筛选新型疗法,因为目前的体外 2D 平面单细胞培养模型不能准确预测临床疗效。我们在此基于球体工程设计了一种新型的人类体外 3D 共培养模型,用于研究(乳腺或前列腺)癌细胞和人骨髓基质细胞的动态细胞数量,并筛选常见抗癌药物顺铂的化疗效果和特异性。骨转移球体(BMS)在 24 小时内迅速形成,而在延长培养时间后,乳腺与前列腺癌 BMS 的形态在大小和圆度方面存在差异。在形成 BMS 之前对细胞类型进行预染色,可实现共焦成像和长达 7 天的 BMS 培养的球体内部细胞动力学的定量图像分析。我们发现 BMS 中的癌细胞比 2D 对照培养物增殖更快,对顺铂治疗的敏感性更低。基于这些发现和我们方法的多功能性,BMS 代表了一种可行的用于筛选新的骨癌转移治疗方法的 3D 体外模型。
