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大规模生产的微孔硅膜,用于特定白细胞亚群的分离、免疫表型分析以及体外个性化免疫调节药物筛选。

Mass-producible microporous silicon membranes for specific leukocyte subset isolation, immunophenotyping, and personalized immunomodulatory drug screening in vitro.

机构信息

Department of Mechanical Engineering, University of Michigan, Ann Arbor, Michigan 48109, USA.

出版信息

Lab Chip. 2019 Sep 10;19(18):3065-3076. doi: 10.1039/c9lc00315k.

Abstract

Widespread commercial and clinical adaptation of biomedical microfluidic technology has been limited in large part due to the lack of mass producibility of polydimethylsiloxane (PDMS) and glass-based devices commonly as reported in the literature. Here, we present a batch-fabricated, robust, and mass-producible immunophenotyping microfluidic device using silicon micromachining processes. Our Si and glass-based microfluidic device, named the silicon microfluidic immunophenotyping assay (SiMIPA), consists of a highly porous (∼40%) silicon membrane that can selectively separate microparticles below a certain size threshold. The device is capable of isolating and stimulating specific leukocyte populations, and allows for measuring their secretion of cell signaling proteins by means of a no-wash homogeneous chemiluminescence-based immunoassay. The high manufacturing throughput (∼170 devices per wafer) makes a large quantity of SiMIPA chips readily available for clinically relevant applications, which normally require large dataset acquisitions for statistical accuracy. With 30 SiMIPA chips, we performed in vitro immunomodulatory drug screening on isolated leukocyte subsets, yielding 5 data points at 6 drug concentrations. Furthermore, the excellent structural integrity of the device allowed for samples and reagents to be loaded using a micropipette, greatly simplifying the experimental protocol.

摘要

由于在文献中普遍报道的商业和临床应用中缺乏聚二甲基硅氧烷(PDMS)和玻璃基器件的大规模生产能力,生物医学微流控技术的广泛商业和临床应用在很大程度上受到限制。在这里,我们使用硅微加工工艺展示了一种批量制造的、坚固的、可大规模生产的免疫表型微流控器件。我们的硅基和玻璃基微流控器件,名为硅微流控免疫表型分析(SiMIPA),由高度多孔(约 40%)的硅膜组成,能够选择性地分离小于一定尺寸阈值的微颗粒。该器件能够分离和刺激特定的白细胞群体,并通过无洗涤均相化学发光免疫分析来测量它们分泌的细胞信号蛋白。高制造吞吐量(每个晶圆约 170 个器件)使得大量的 SiMIPA 芯片可用于临床相关应用,这些应用通常需要大量数据集采集以确保统计准确性。使用 30 个 SiMIPA 芯片,我们对分离的白细胞亚群进行了体外免疫调节药物筛选,在 6 种药物浓度下得到了 5 个数据点。此外,该器件具有出色的结构完整性,允许使用微量移液器加载样品和试剂,大大简化了实验方案。

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