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三阴性乳腺癌患者来源肿瘤球体的多功能分析用于疾病建模。

Multifunctional profiling of triple-negative breast cancer patient-derived tumoroids for disease modeling.

机构信息

Protein Fluidics, Inc., USA.

Molecular Devices, LLC, USA.

出版信息

SLAS Discov. 2022 Apr;27(3):191-200. doi: 10.1016/j.slasd.2022.01.006. Epub 2022 Feb 4.

DOI:10.1016/j.slasd.2022.01.006
PMID:35124274
Abstract

3D cell models derived from patient tumors are highly translational tools that can recapitulate the complex genetic and molecular compositions of solid cancers and accelerate identification of drug targets and drug testing. However, the complexity of performing assays with such models remains a hurdle for their wider adoption. In the present study, we describe methods for processing and multi-functional profiling of tumoroid samples to test compound effects using a novel flowchip system in combination with high content imaging and metabolite analysis. Tumoroids were formed from primary cells isolated from a patient-derived tumor explant, TU-BcX-4IC, that represents metaplastic breast cancer with a triple-negative breast cancer subtype. Assays were performed in a microfluidics-based device (Pu⋅MA System) that allows automated exchange of media and treatments of tumoroids in a tissue culture incubator environment. Multi-functional assay profiling was performed on tumoroids treated with anti-cancer drugs. High-content imaging was used to evaluate drug effects on cell viability and expression of E-cadherin and CD44. Lactate secretion was used to measure tumoroid metabolism as a function of time and drug concentration. Observed responses included loss of cell viability, decrease in E-cadherin expression, and increase of lactate production. Importantly, the tumoroids were sensitive to romidepsin and trametinib, while showed significantly reduced sensitivity to paclitaxel and cytarabine, consistent with the primary tumor response. These methods for multi-parametric profiling of drug effects in patient-derived tumoroids provide an in depth understanding of drug sensitivity of individual tumor types, with important implications for the future development of personalized medicine.

摘要

源自患者肿瘤的 3D 细胞模型是高度转化的工具,能够重现实体瘤复杂的遗传和分子组成,并加速药物靶点的鉴定和药物测试。然而,使用此类模型进行检测的复杂性仍然是其更广泛应用的障碍。在本研究中,我们描述了处理和多功能分析肿瘤球样本的方法,以使用新型流片系统结合高内涵成像和代谢物分析来测试化合物的影响。肿瘤球是从源自患者衍生的肿瘤外植体 TU-BcX-4IC 的原代细胞中形成的,该肿瘤外植体代表具有三阴性乳腺癌亚型的间变性乳腺癌。在基于微流控的设备(Pu⋅MA 系统)中进行了检测,该设备允许在组织培养孵育箱环境中自动更换培养基和处理肿瘤球。对用抗癌药物处理的肿瘤球进行多功能分析。高内涵成像用于评估药物对细胞活力和 E-钙黏蛋白和 CD44 表达的影响。乳酸分泌用于测量肿瘤球代谢随时间和药物浓度的变化。观察到的反应包括细胞活力丧失、E-钙黏蛋白表达减少和乳酸生成增加。重要的是,肿瘤球对罗米地辛和曲美替尼敏感,而对紫杉醇和阿糖胞苷的敏感性显著降低,与原发肿瘤的反应一致。这些用于患者来源的肿瘤球中药物作用的多参数分析方法提供了对个体肿瘤类型药物敏感性的深入了解,对个性化医学的未来发展具有重要意义。

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