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首页> 外文期刊>PLoS One >Microfluidics sorting enables the isolation of an intact cellular pair complex of CD8 + T cells and antigen-presenting cells in a cognate antigen recognition-dependent manner
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Microfluidics sorting enables the isolation of an intact cellular pair complex of CD8 + T cells and antigen-presenting cells in a cognate antigen recognition-dependent manner

机译:微流体分选使得能够以同源抗原识别依赖性方式分离CD8 + T细胞和抗原呈递细胞的完整细胞对复合物

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Adaptive immune responses begin with cognate antigen presentation-dependent specific interaction between T cells and antigen-presenting cells. However, there have been limited reports on the isolation and analysis of these cellular complexes of T cell-antigen-presenting cell (T/APC). In this study, we successfully isolated intact antigen-specific cellular complexes of CD8 + T/APC by utilizing a microfluidics cell sorter. Using ovalbumin (OVA) model antigen and OT-I-derived OVA-specific CD8 + T cells, we analyzed the formation of antigen-specific and antigen-non-specific T/APC cellular complexes and revealed that the antigen-specific T/APC cellular complex was highly stable than the non-specific one, and that the intact antigen-specific T/APC complex can be retrieved as well as enriched using a microfluidics sorter, but not a conventional cell sorter. The single T/APC cellular complex obtained can be further analyzed for the sequences of T cell receptor Vα and Vβ genes as well as cognate antigen information simultaneously. These results suggested that this approach can be applied for other antigen and CD8 + T cells of mice and possibly those of humans. We believe that this microfluidics sorting method of the T/APC complex will provide useful information for future T cell immunology research.
机译:自适应免疫应答从T细胞和抗原呈递细胞之间的同源抗原呈递依赖性特异性相互作用开始。然而,关于T细胞 - 抗原呈递细胞(T / APC)的这些细胞复合物的分离和分析存在有限的报道。在这项研究中,我们通过利用微流体细胞分选器成功地分离CD8 + T / APC的完整抗原特异性细胞复合物。使用卵烧(OVA)模型抗原和OT-I衍生的OVA特异性CD8 + T细胞,我们分析了抗原特异性和抗原 - 非特异性T / APC细胞复合物的形成,并揭示了抗原特异性T / APC细胞复合物高于非特异性稳定性,并且可以检索完整的抗原特异性T / APC复合物以及使用微流体分选器来富集,但不是常规的细胞分选。获得的单个T / APC细胞复合物可以进一步分析T细胞受体Vα和Vβ基因的序列以及同时的同源抗原信息。这些结果表明这种方法可以应用于小鼠的其他抗原和CD8 + T细胞和可能是人类的方法。我们认为,T / APC复合物的这种微流体分选方法将为未来T细胞免疫学研究提供有用的信息。

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