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首页> 外文期刊>International Immunology >Impact of CD8–MHC class I interaction in detection and sorting efficiencies of antigen-specific T cells using MHC class I/peptide multimers: contribution of pMHC valency
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Impact of CD8–MHC class I interaction in detection and sorting efficiencies of antigen-specific T cells using MHC class I/peptide multimers: contribution of pMHC valency

机译:CD8–MHC I类相互作用对使用MHC I类/肽多聚体的抗原特异性T细胞的检测和分选效率的影响:pMHC价的贡献

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摘要

Recombinant soluble multimeric forms of MHC class I molecules loaded with antigenic peptides (pMHC) have turned out to be particularly useful to detect and isolate specific T cells. These applications both rely on the oligomerization of pMHC monomers in order to compensate for their inherent low affinity for the TCR. In this study, we have evaluated the precise contribution of CD8–pMHC interaction on the specificity and sorting efficiency of pMHC multimers according to their degree of oligomerization. To this end several wild-type versus mutated pMHC complexes (A*0201, B*0701, B*0801, B*3501) carrying point mutations known to reduce (245V mutants) or to abrogate (227,8KA mutants) CD8–pMHC interaction and showing various degrees of valency have been used. We show that irrespective of the HLA allele tested, 245V mutation strongly improves the binding specificity and immunomagnetic sorting efficiency of pMHC multimers. Our results also indicate that the contribution of CD8 to the binding of pMHC multimers to specific CD8+ T cells is inversely correlated to the degree of pMHC oligomerization. Consequently, efficient staining or specific sorting of high-affinity T cells (i.e. CD8 independent) can only be achieved using 227,8KA pMHC complexes with low-order oligomerization.
机译:事实证明,装载有抗原肽(pMHC)的MHC I类分子的重组可溶性多聚体形式特别适用于检测和分离特定的T细胞。这些应用都依赖于pMHC单体的低聚反应,以补偿它们对TCR固有的低亲和力。在这项研究中,我们评估了CD8-pMHC相互作用对pMHC多聚体的寡聚程度及其特异性和分选效率的精确贡献。为此,已知几种野生型与突变型pMHC复合物(A * 0201,B * 0701,B * 0801,B * 3501)携带点突变,已知可减少(245V突变体)或消除(227,8KA突变体)CD8–pMHC相互作用并显示出不同价态。我们表明,无论测试的HLA等位基因如何,245V突变都可大大提高pMHC多聚体的结合特异性和免疫磁分选效率。我们的研究结果还表明,CD8对pMHC多聚体与特定CD8 + T细胞结合的贡献与pMHC寡聚程度成反比。因此,仅使用具有低阶低聚的227,8KA pMHC复合物才能实现高亲和力T细胞(即独立于CD8)的有效染色或特异性分选。

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