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Secondary anchor targeted cell release

机译:次生锚定靶细胞释放

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Personalized medicine offers the promise of tailoring therapy to patients, based on their cellular biomarkers. To achieve this goal, cellular profiling systems are needed that can quickly and efficiently isolate specific cell types without disrupting cellular biomarkers. Here we describe the development of a unique platform that facilitates gentle cell capture via a secondary, surface-anchoring moiety, and cell release. The cellular capture system consists of a glass surface functionalized with APTES, d-desthiobiotin, and streptavidin. Biotinylated mCD11b and hIgG antibodies are used to capture mouse macrophages (RAW 264.7) and human breast cancer (MCF7-GFP) cell lines, respectively. The surface functionalization is optimized by altering assay components, such as streptavidin, d-desthiobiotin, and APTES, to achieve cell capture on 80% of the functionalized surface and cell release upon biotin treatment. We also demonstrate an ability to capture 50% of target cells within a dual-cell mixture. This engineering advancement is a critical step towards achieving cell isolation platforms for personalized medicine. Biotechnol. Bioeng. 2015;112: 2214-2227. (c) 2015 Wiley Periodicals, Inc.
机译:个性化医学有望根据患者的细胞生物标记物为患者量身定制治疗方案。为了实现这一目标,需要能够在不破坏细胞生物标志物的情况下快速有效地分离特定细胞类型的细胞谱分析系统。在这里,我们描述了一个独特的平台的开发,该平台有助于通过次要的,表面锚定的部分和细胞释放来轻柔地捕获细胞。细胞捕获系统由用APTES,d-脱硫生物素和链霉亲和素功能化的玻璃表面组成。生物素化的mCD11b和hIgG抗体分别用于捕获小鼠巨噬细胞(RAW 264.7)和人乳腺癌(MCF7-GFP)细胞系。通过改变分析成分(例如链霉亲和素,d-脱硫生物素和APTES)来优化表面功能化,以实现在80%的功能化表面捕获细胞并在生物素处理后释放细胞。我们还展示了捕获双细胞混合物中50%靶细胞的能力。工程上的进步是朝着实现个性化医学的细胞分离平台迈出的关键一步。生物技术。生恩2015; 112:2214-2227。 (c)2015年威利期刊有限公司

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