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基于链霉亲和素的肽-MHC 低聚体(四聚体)与细胞表面 TCR 的相互作用。

Interaction of streptavidin-based peptide-MHC oligomers (tetramers) with cell-surface TCRs.

机构信息

Department of Biochemistry, University of Illinois, Urbana-Champaign, Urbana, IL 61801, USA.

出版信息

J Immunol. 2011 Dec 15;187(12):6281-90. doi: 10.4049/jimmunol.1101734. Epub 2011 Nov 18.

Abstract

The binding of oligomeric peptide-MHC (pMHC) complexes to cell surface TCR can be considered to approximate TCR-pMHC interactions at cell-cell interfaces. In this study, we analyzed the equilibrium binding of streptavidin-based pMHC oligomers (tetramers) and their dissociation kinetics from CD8(pos) T cells from 2C-TCR transgenic mice and from T cell hybridomas that expressed the 2C TCR or a high-affinity mutant (m33) of this TCR. Our results show that the tetramers did not come close to saturating cell-surface TCR (binding only 10-30% of cell-surface receptors), as is generally assumed in deriving affinity values (K(D)), in part because of dissociative losses from tetramer-stained cells. Guided by a kinetic model, the oligomer dissociation rate and equilibrium constants were seen to depend not only on monovalent association and dissociation rates (k(off) and k(on)), but also on a multivalent association rate (μ) and TCR cell-surface density. Our results suggest that dissociation rates could account for the recently described surprisingly high frequency of tetramer-negative, functionally competent T cells in some T cell responses.

摘要

寡聚肽-MHC(pMHC)复合物与细胞表面 TCR 的结合可以被认为近似于细胞-细胞界面处 TCR-pMHC 的相互作用。在这项研究中,我们分析了基于链霉亲和素的 pMHC 寡聚体(四聚体)与来自 2C-TCR 转基因小鼠的 CD8(+) T 细胞以及表达 2C TCR 或该 TCR 的高亲和力突变体(m33)的 T 细胞杂交瘤的平衡结合及其解离动力学。我们的结果表明,四聚体并没有接近饱和细胞表面 TCR(仅结合细胞表面受体的 10-30%),这在推导亲和力值(K(D))时通常是假设的,部分原因是四聚体染色细胞的解离损失。通过动力学模型指导,我们发现寡聚体解离速率和平衡常数不仅取决于单价结合和解离速率(k(off)和 k(on)),还取决于多价结合速率(μ)和 TCR 细胞表面密度。我们的结果表明,解离速率可以解释最近描述的一些 T 细胞反应中令人惊讶的高比例四聚体阴性、功能上有能力的 T 细胞的频率。

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