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基于微流控的动态BH3分析可预测抗癌治疗效果。

Microfluidic-based dynamic BH3 profiling predicts anticancer treatment efficacy.

作者信息

Manzano-Muñoz Albert, Yeste José, Ortega María A, Martín Fernando, López Anna, Rosell Jordi, Castro Sandra, Serrano César, Samitier Josep, Ramón-Azcón Javier, Montero Joan

机构信息

Nanobioengineering Group, Institute for Bioengineering of Catalonia (IBEC), Barcelona Institute of Science and Technology (BIST), Barcelona, Spain.

Biosensors for Bioengineering Group, Institute for Bioengineering of Catalonia (IBEC), Barcelona Institute of Science and Technology (BIST), Barcelona, Spain.

出版信息

NPJ Precis Oncol. 2022 Dec 1;6(1):90. doi: 10.1038/s41698-022-00333-0.

Abstract

Precision medicine is starting to incorporate functional assays to evaluate anticancer agents on patient-isolated tissues or cells to select for the most effective. Among these new technologies, dynamic BH3 profiling (DBP) has emerged and extensively been used to predict treatment efficacy in different types of cancer. DBP uses synthetic BH3 peptides to measure early apoptotic events ('priming') and anticipate therapy-induced cell death leading to tumor elimination. This predictive functional assay presents multiple advantages but a critical limitation: the cell number requirement, that limits drug screening on patient samples, especially in solid tumors. To solve this problem, we developed an innovative microfluidic-based DBP (µDBP) device that overcomes tissue limitations on primary samples. We used microfluidic chips to generate a gradient of BIM BH3 peptide, compared it with the standard flow cytometry based DBP, and tested different anticancer treatments. We first examined this new technology's predictive capacity using gastrointestinal stromal tumor (GIST) cell lines, by comparing imatinib sensitive and resistant cells, and we could detect differences in apoptotic priming and anticipate cytotoxicity. We then validated µDBP on a refractory GIST patient sample and identified that the combination of dactolisib and venetoclax increased apoptotic priming. In summary, this new technology could represent an important advance for precision medicine by providing a fast, easy-to-use and scalable microfluidic device to perform DBP in situ as a routine assay to identify the best treatment for cancer patients.

摘要

精准医学开始纳入功能测定,以在患者分离的组织或细胞上评估抗癌药物,从而选择最有效的药物。在这些新技术中,动态BH3分析(DBP)应运而生,并被广泛用于预测不同类型癌症的治疗效果。DBP使用合成的BH3肽来测量早期凋亡事件(“启动”),并预测治疗诱导的细胞死亡,从而导致肿瘤消除。这种预测性功能测定具有多个优点,但也有一个关键限制:对细胞数量的要求,这限制了对患者样本进行药物筛选,尤其是在实体瘤中。为了解决这个问题,我们开发了一种基于微流控的创新DBP(µDBP)设备,该设备克服了对原发性样本的组织限制。我们使用微流控芯片生成BIM BH3肽梯度,将其与基于标准流式细胞术的DBP进行比较,并测试了不同的抗癌治疗方法。我们首先通过比较伊马替尼敏感和耐药细胞,使用胃肠道间质瘤(GIST)细胞系检验了这项新技术的预测能力,并且我们能够检测到凋亡启动的差异并预测细胞毒性。然后,我们在一个难治性GIST患者样本上验证了µDBP,并确定了达可替尼和维奈托克的联合使用增加了凋亡启动。总之,这项新技术可为精准医学带来重要进展,它提供了一种快速、易用且可扩展的微流控设备,可作为常规测定原位进行DBP,以确定癌症患者的最佳治疗方案。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/af90/9715649/c06f32112309/41698_2022_333_Fig1_HTML.jpg

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