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Binding Strength and Dynamics of Invariant Natural Killer Cell T Cell Receptor/CD1d-Glycosphingolipid Interaction on Living Cells by Single Molecule Force Spectroscopy*

机译:单分子力谱分析法测定不变的自然杀伤细胞T细胞受体/ CD1d-糖鞘脂相互作用在活细胞上的结合强度和动力学*

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摘要

Invariant natural killer T (iNKT) cells are a population of T lymphocytes that play an important role in regulating immunity to infection and tumors by recognizing endogenous and exogenous CD1d-bound lipid molecules. Using soluble iNKT T cell receptor (TCR) molecules, we applied single molecule force spectroscopy for the investigation of the iNKT TCR affinity for human CD1d molecules loaded with glycolipids differing in the length of the phytosphingosine chain using either recombinant CD1d molecules or lipid-pulsed THP1 cells. In both settings, the dissociation of the iNKT TCR from human CD1d molecules loaded with the lipid containing the longer phytosphingosine chain required higher unbinding forces compared with the shorter phytosphingosine lipid. Our findings are discussed in the context of previous results obtained by surface plasmon resonance measurements. We present new insights into the energy landscape and the kinetic rate constants of the iNKT TCR/human CD1d-glycosphingolipid interaction and emphasize the unique potential of single molecule force spectroscopy on living cells.
机译:不变的自然杀伤性T细胞(iNKT)是一群T淋巴细胞,它们通过识别内源性和外源性CD1d结合的脂质分子在调节对感染和肿瘤的免疫力中起重要作用。我们使用可溶性iNKT T细胞受体(TCR)分子,通过重组CD1d分子或脂质脉冲THP1,应用单分子力光谱法研究了iNKT TCR对载有糖脂的人CD1d分子的亲和力,这些糖脂在植物鞘氨醇链的长度上不同。细胞。在这两种情况下,与较短的植物鞘氨醇脂质相比,iNKT TCR与负载了含有较长植物鞘氨醇链的脂质的人CD1d分子的解离需要更高的去结合力。我们的发现将在通过表面等离振子共振测量获得的先前结果的背景下进行讨论。我们提出了对iNKT TCR /人CD1d-糖鞘脂相互作用的能级图和动力学速率常数的新见解,并强调了单分子力谱在活细胞上的独特潜力。

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