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单个贴壁细胞的高通量功能分析:水凝胶滴筛法

High-throughput functional profiling of single adherent cells hydrogel drop-screen.

作者信息

Wang Ming, Nai Mui Hoon, Huang Ruby Yun-Ju, Leo Hwa Liang, Lim Chwee Teck, Chen Chia-Hung

机构信息

NUS Graduate School for Integrative Sciences & Engineering, National University of Singapore, 21 Lower Kent Ridge Road, 119077 Singapore and Department of Biomedical Engineering, National University of Singapore, 4 Engineering Drive 3, 117583 Singapore and Institute for Health Innovation and Technology (iHealthtech), MD6, 14 Medical Drive 14-01, 117599 Singapore.

Department of Biomedical Engineering, National University of Singapore, 4 Engineering Drive 3, 117583 Singapore.

出版信息

Lab Chip. 2021 Feb 23;21(4):764-774. doi: 10.1039/d0lc01294g.

Abstract

Single-adherent-cell phenotyping on an extracellular matrix (ECM) is essential to determine cellular biological functions, such as morphological adaptations and biomolecule secretions, correlated to medical treatments and metastasis, yet there is no available platform for such high-throughput screening. Here, a novel hydrogel drop-screen device was developed to rapidly measure large-scale single-cell morphologies and multiple secretions on substrates for phenotype profiling. Single cells were first anchored to microfluidically fabricated gelatin particles providing mechanical stimulations similar to those from ECM in vivo. The cellular morphologies were then examined by quantifying the amount of cytoskeleton expressed on the particles. With droplet encapsulation, adherent single-cell multiplexed secretion analysis of a disintegrin and metalloproteinases (ADAMs) and matrix metalloproteinases (MMPs) was conducted at a throughput of ∼102 cells per second, revealing distinct functional heterogeneities associated with extracellular mechanical stimulations. The level of cell heterogeneity increased with increasing substrate stuffiness. Moreover, because of the promising screening capability, a database related to both nontumorigenic and tumorigenic breast cells (MCF10A, MCF-7, and MDA-MB-231) was constructed. The respective cell distributions and heterogeneities based on the morphologies and secreted bioindicators, such as MMP-2, MMP-3, MMP-9, and ADAM-8, were measured and found to correspond to the progress of tumor metastasis.

摘要

在细胞外基质(ECM)上进行单粘附细胞表型分析对于确定细胞生物学功能至关重要,这些功能如形态适应和生物分子分泌,与医学治疗和转移相关,但目前尚无用于这种高通量筛选的平台。在此,开发了一种新型水凝胶滴筛装置,用于快速测量底物上大规模单细胞形态和多种分泌物以进行表型分析。单细胞首先锚定在微流控制造的明胶颗粒上,这些颗粒提供类似于体内ECM的机械刺激。然后通过量化颗粒上表达的细胞骨架量来检查细胞形态。通过液滴封装,以每秒约102个细胞的通量对去整合素和金属蛋白酶(ADAMs)和基质金属蛋白酶(MMPs)进行粘附单细胞多重分泌分析,揭示了与细胞外机械刺激相关的明显功能异质性。细胞异质性水平随着底物硬度的增加而增加。此外,由于具有良好的筛选能力,构建了一个与非致瘤性和致瘤性乳腺细胞(MCF10A、MCF-7和MDA-MB-231)相关的数据库。基于形态和分泌的生物指标(如MMP-2、MMP-3、MMP-9和ADAM-8)测量了各自的细胞分布和异质性,发现其与肿瘤转移进程相对应。

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