化学
微流控
微流控芯片
药品
灵敏度(控制系统)
色谱法
体外
稀释
肺癌
纳米技术
药理学
生物化学
内科学
医学
材料科学
物理
电子工程
工程类
热力学
作者
Chenchen Zhang,Kuo Tian,Zixun Meng,Jianing Zhang,Yihong Lu,Li Tan,Mei Zhang,Danke Xu
出处
期刊:Talanta
[Elsevier BV]
日期:2024-05-29
卷期号:277: 126298-126298
标识
DOI:10.1016/j.talanta.2024.126298
摘要
Combination drug therapy represents an effective strategy for treating certain drug-resistant and intractable cancer cases. However, determining the optimal combination of drugs and dosages is challenging due to clonal diversity in patients' tumors and the lack of rapid drug sensitivity evaluation methods. Microfluidic technology offers promising solutions to this issue. In this study, we propose a versatile microfluidic chip platform capable of integrating all processes, including dilution, treatment, and detection, for in vitro drug sensitivity assays. This platform innovatively incorporates several modules, including automated discrete drug logarithmic concentration generation, on-chip cell perfusion culture, and parallel drug treatments of cancer cell models. Moreover, it is compatible with microplate readers or high-content imaging systems for swift detection and automated monitoring, simplifying on-chip drug evaluation. Proof of concept is demonstrated by assessing the in vitro potency of two drugs, cisplatin, and etoposide, against the lung adenocarcinoma A549 cell line, under both single-drug and combination treatment conditions. The findings reveal that, compared to conventional microplate approaches with static cultivation, this on-chip automated perfusion bioassays yield comparable IC50 values with lower variation and a 50% reduction in drug preparation time. This versatile dilution-treatment-detection microfluidic platform offers a promising tool for rapid and precise drug assessments, facilitating in vitro drug sensitivity evaluation in personalized cancer chemotherapy.
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