首页> 外文期刊>Journal of Immunological Methods >Probing T cell membrane organization using dimeric MHC-Ig complexes.
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Probing T cell membrane organization using dimeric MHC-Ig complexes.

机译:使用二聚体MHC-Ig复合物探测T细胞膜组织。

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摘要

In this report, we review a novel method for probing the membrane organization of T cells using dimeric major histocompatibility complexes (MHC), MHC-Ig. MHC-Ig complexes are useful reagents for quantitative analysis of binding data since their valency is controlled. These complexes can be easily labeled and loaded with a variety of peptides. A binding assay using these dimers and quantitative analysis of the MHC-Ig dimer-T cell binding curves is described in detail. Using this approach, we show that the organization of TCR on activated T cells is different from TCR organization on nai;ve T cells. The implications of these findings are discussed with regards to current models of T cell recognition. This analysis offers insight into how T cell controls their biological range of responsiveness. Specifically, these findings reveal the biophysical basis of the ability of activated T cells to recognize low amounts of antigen independent of costimulation.
机译:在本报告中,我们回顾了一种使用二聚体主要组织相容性复合体(MHC),MHC-Ig探测T细胞膜组织的新方法。 MHC-Ig复合物是有效的试剂,可用于定量分析结合数据,因为它们的化合价受到控制。这些复合物可以轻松地标记并装载各种肽。详细描述了使用这些二聚体的结合测定和MHC-Ig二聚体-T细胞结合曲线的定量分析。使用这种方法,我们证明了活化T细胞上TCR的组织不同于天然T细胞上TCR的组织。关于当前的T细胞识别模型,讨论了这些发现的含义。该分析提供了有关T细胞如何控制其生物学反应范围的见解。具体而言,这些发现揭示了活化的T细胞识别少量抗原的能力的生物物理基础,而与共刺激无关。

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