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FACS isolation of low percentage human antigen-specific CD8~+ T cells based on activation-induced CD3 and CD8 downregulation

机译:基于活化诱导的CD3和CD8下调的低百分比人抗原特异性CD8 + T细胞的低百分比人抗原特异性CD8 + T细胞的分离

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摘要

As T cell activation leads to downregulation of T cell receptor (TCR) and coreceptor CD8, we developed a novel FACS-based sorting method to enrich activated antigen-specific CD8~+ T cells. Using multiple established or low percentage T cell cultures, with either single antigen specificity or multiple influenza A virus antigen specificities, we have optimized the sorting method for T cell activation time and stimulating antigen dose. We have also sorted various numbers of antigen-specific CD8~+T cells into 96-well plates to demonstrate these T cells are capable of expanding into nearly pure CD~+ T cell lines. Our approach has the advantage of sorting antigen-specific T cells without knowing their specific antigenic epitopes or restricting HLA. We believe this method can be very helpful for successfully establishing CD8~+ T cell lines for various purpose, including immunotherapy.
机译:作为T细胞活化导致T细胞受体(TCR)和团簇CD8的下调,我们开发了一种基于FAC的基于FACS的分选方法,以丰富活化的抗原特异性CD8 + T细胞。 使用多种建立或低百分比的T细胞培养物,具有单一抗原特异性或多种流感病毒抗原特异性,我们已经优化了T细胞活化时间和刺激抗原剂量的分选方法。 我们还将各种数量的抗原特异性CD8〜+ T细胞分为96孔板,以证明这些T细胞能够扩展到几乎纯的CD〜+ T细胞系中。 我们的方法具有在不知道其特异性抗原表位或限制HLA的情况下对抗原特异性T细胞进行分类。 我们认为,这种方法对于成功建立CD8〜+ T细胞系来为各种目的而有用,包括免疫疗法。

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