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Label-free Electronic Detection of the Antigen-Specific T-Cell Immune Response

机译:抗原特异性T细胞免疫反应的无标记电子检测

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摘要

Detection of antigen-specific T-cells is critical for diagnostic assessment and design of therapeutic strategies for many disease states. Effective monitoring of these cells requires technologies that assess their numbers as well as functional response. Current detection of antigen-specific T-cells involves flow cytometry and functional assays and requires fluorescently labeled, soluble forms of peptide-loaded major histocompatability complexes (MHC). We demonstrate that nanoscale solid-state complementary metal-oxide-semiconductor (CMOS) technology can be employed to allow direct, label-free electronic detection of antigen-specific T-cell responses within seconds after stimulation. Our approach relies on detection of extracellular acidification arising from a small number of T-cells (as few as ~200), whose activation is induced by triggering the T-cell antigen receptor. We show that T-cell triggering by a nonspecific anti-CD3 stimulus can be detected within 10 s after exposure to the stimulus. In contrast, antigen-specific T-cell responses are slower with response times greater than 40 s after exposure to peptide/MHC agonists. The speed and sensitivity of this technique has the potential to elucidate new understandings of the kinetics of activation-induced T-cell responses. This combined with its ease of integration into conventional electronics potentially enable rapid clinical testing and high-throughput epitope and drug screening.
机译:抗原特异性T细胞的检测对于多种疾病的诊断评估和治疗策略设计至关重要。有效监控这些细胞需要评估其数量以及功能反应的技术。当前对抗原特异性T细胞的检测涉及流式细胞术和功能测定,并且需要荧光标记的可溶性形式的肽加载的主要组织相容性复合物(MHC)。我们证明,纳米级固态互补金属氧化物半导体(CMOS)技术可以用于允许刺激后几秒钟内直接,无标记的抗原特异性T细胞反应的电子检测。我们的方法依赖于检测少量T细胞(少至200个)引起的细胞外酸化,其活化是通过触发T细胞抗原受体来诱导的。我们表明,由非特异性抗CD3刺激引起的T细胞触发可在暴露于刺激后10 s内被检测到。相反,暴露于肽/ MHC激动剂后,抗原特异性T细胞反应较慢,反应时间大于40 s。这项技术的速度和敏感性有可能阐明对激活诱导的T细胞反应动力学的新认识。这加上其易于集成到常规电子设备中的潜力,有可能实现快速的临床测试以及高通量的表位和药物筛选。

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