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Digital microfluidic immunocytochemistry in single cells

机译:单细胞中的数字微流免疫细胞化学

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We report a new technique called Digital microfluidic Immunocytochemistry in Single Cells (DISC). DISC automates protocols for cell culture, stimulation and immunocytochemistry, enabling the interrogation of protein phosphorylation on pulsing with stimulus for as little as 3 s. DISC was used to probe the phosphorylation states of platelet-derived growth factor receptor (PDGFR) and the downstream signalling protein, Akt, to evaluate concentration-and time-dependent effects of stimulation. The high time resolution of the technique allowed for surprising new observations-for example, a 10 s pulse stimulus of a low concentration of PDGF is sufficient to cause >30% of adherent fibroblasts to commit to Akt activation. With the ability to quantitatively probe signalling events with high time resolution at the single-cell level, we propose that DISC may be an important new technique for a wide range of applications, especially for screening signalling responses of a heterogeneous cell population.
机译:我们报告了一种称为单细胞数字微流免疫细胞化学(DISC)的新技术。 DISC使细胞培养,刺激和免疫细胞化学操作自动化,从而能够在短短3 s的刺激下询问蛋白磷酸化。 DISC用于检测血小板衍生的生长因子受体(PDGFR)和下游信号蛋白Akt的磷酸化状态,以评估刺激的浓度和时间依赖性。该技术的高时间分辨率可带来令人惊讶的新发现-例如,低浓度PDGF的10 s脉冲刺激足以引起> 30%的粘附成纤维细胞发生Akt活化。凭借在单细胞水平上以高时间分辨率定量探测信号事件的能力,我们提出DISC可能是一项重要的新技术,适用于广泛的应用,尤其是用于筛选异质细胞群体的信号反应。

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