Mercier Blandine C, Cottalorda Anne, Coupet Charles-Antoine, Marvel Jacqueline, Bonnefoy-Bérard Nathalie
Université de Lyon, Lyon, France.
J Immunol. 2009 Feb 15;182(4):1860-7. doi: 10.4049/jimmunol.0801167.
TLR are involved in the detection of microbial infection as well as endogenous ligands that signal tissue and cell damage in mammals. This recognition plays an essential role in innate immune response and the initiation of adaptive immune response. We have previously shown that murine CD8 T cells express TLR2, and that costimulation of Ag-activated CD8 T cells with TLR2 ligands enhances their proliferation, survival, and effector functions. We also demonstrated that TLR2 engagement on CD8 T cells significantly reduces their need for costimulatory signals delivered by APC. We show in this study that TLR2 engagement on CD8 T cells lowers the Ag concentration required for optimal activation, and converts a partial activation into a productive process leading to a significant expansion of cells. Using altered peptide ligands, we demonstrate that TLR2 engagement increases CD8 T cell activation and enables the generation of functional memory cells in response to a low TCR signal. This increased activation is associated with an augmented activation of the PI3K. Taken together, our results demonstrate that TLR2 engagement on CD8 T cells lowers their activation threshold for TCR signal strength and enables efficient memory cell generation in response to a weak TCR signal.
Toll样受体(TLR)参与检测哺乳动物中的微生物感染以及指示组织和细胞损伤的内源性配体。这种识别在先天免疫应答和适应性免疫应答的启动中起着至关重要的作用。我们之前已经表明,小鼠CD8 T细胞表达TLR2,并且用TLR2配体共刺激抗原激活的CD8 T细胞可增强其增殖、存活和效应功能。我们还证明,CD8 T细胞上的TLR2结合显著降低了它们对由抗原呈递细胞(APC)传递的共刺激信号的需求。我们在本研究中表明,CD8 T细胞上的TLR2结合降低了最佳激活所需的抗原浓度,并将部分激活转化为导致细胞显著扩增的有效过程。使用改变的肽配体,我们证明TLR2结合增加了CD8 T细胞的激活,并能够在低TCR信号响应下产生功能性记忆细胞。这种增加的激活与PI3K的增强激活有关。综上所述,我们的结果表明,CD8 T细胞上的TLR2结合降低了它们对TCR信号强度的激活阈值,并能够在弱TCR信号响应下高效产生记忆细胞。
