Department of Molecular Medicine, Istituto Pasteur-Fondazione Cenci Bolognetti, "Sapienza" University of Rome Rome, Italy.
Front Immunol. 2013 Jan 9;3:408. doi: 10.3389/fimmu.2012.00408. eCollection 2012.
The negative regulation of adaptive immunity is relevant to maintain lymphocyte homeostasis. Several studies on natural killer (NK) cells have shown a previously unappreciated immunomodulatory role, as they can negatively regulate T cell-mediated immune responses by direct killing and by secretion of inhibitory cytokines. The molecular mechanisms of T cell suppression by NK cells, however, remained elusive. Only in the last few years has it become evident that, upon activation, human T cells express MICA-B, ULBP1-3, and PVR, ligands of the activating receptors NKG2D and DNAM-1, respectively. Their expression renders T cells targets of NK cell lysis, representing a new mechanism taking part to the negative regulation of T cell responses. Studies on the expression of NKG2D and DNAM-1 ligands on T cells have also contributed in understanding that the activation of ATM (ataxia-telangiectasia, mutated)/ATR (ATM/Rad3-related) kinases and the DNA damage response is a common pathway regulating the expression of activating ligands in different types of cells and under different conditions. The functional consequences of NKG2D and DNAM-1 ligand expression on activated T cells are discussed in the context of physiologic and pathologic processes such as infections, autoimmunity, and graft versus host disease.
适应性免疫的负调控与维持淋巴细胞稳态有关。几项关于自然杀伤 (NK) 细胞的研究表明,它们具有以前未被重视的免疫调节作用,因为它们可以通过直接杀伤和分泌抑制性细胞因子来负调控 T 细胞介导的免疫反应。然而,NK 细胞抑制 T 细胞的分子机制仍不清楚。直到最近几年,人们才发现,人类 T 细胞在激活后表达 MICA-B、ULBP1-3 和 PVR,分别是激活受体 NKG2D 和 DNAM-1 的配体。它们的表达使 T 细胞成为 NK 细胞裂解的靶标,这代表了参与 T 细胞反应负调控的新机制。关于 T 细胞上 NKG2D 和 DNAM-1 配体表达的研究也有助于理解,ATM(共济失调毛细血管扩张症突变体/ATR(ATM/Rad3 相关)激酶)和 DNA 损伤反应的激活是调节不同类型细胞和不同条件下激活配体表达的共同途径。在感染、自身免疫和移植物抗宿主病等生理和病理过程中,讨论了 NKG2D 和 DNAM-1 配体在激活的 T 细胞上的表达的功能后果。
