Dhein J, Walczak H, Bäumler C, Debatin K M, Krammer P H
Tumorimmunology Program, German Cancer Research Center, Heidelberg.
Nature. 1995 Feb 2;373(6513):438-41. doi: 10.1038/373438a0.
The APO-1/(Fas/CD95) cell surface receptor is a member of the nerve growth factor (NGF)/tumour necrosis factor (TNF) receptor superfamily and mediates apoptosis. Peripheral activated T cells (ATC) from lymphoproliferation (lpr/lpr) mutant mice that express a reduced number of APO-1 receptors have a defect in T-cell receptor (TCR)-induced apoptosis. This suggests that TCR-induced apoptosis involves APO-1. We tested this hypothesis in various human T cells: (1) malignant Jurkat cells, (2) an alloreactive T-cell clone (S13), and (3) peripheral ATC. TCR triggering through immobilized anti-CD3 antibodies or Staphylococcus enterotoxin B (SEB) superantigen induced expression of the APO-1 ligand and apoptosis in these cells. Anti-CD3-induced apoptosis of Jurkat cells was demonstrated even in single-cell cultures. In all cases apoptosis was substantially inhibited by blocking anti-APO-1 antibody fragments and soluble APO-1 receptor decoys. The APO-1 ligand was found in the supernatant of activated Jurkat cells as a soluble cytokine. We propose that TCR-induced apoptosis in ATC can occur through an APO-1 ligand-mediated autocrine suicide. These results provide a mechanism for suppression of the immune response and for peripheral tolerance by T-cell deletion.
APO-1/(Fas/CD95)细胞表面受体是神经生长因子(NGF)/肿瘤坏死因子(TNF)受体超家族的成员,可介导细胞凋亡。来自淋巴细胞增殖(lpr/lpr)突变小鼠的外周活化T细胞(ATC)表达的APO-1受体数量减少,在T细胞受体(TCR)诱导的细胞凋亡方面存在缺陷。这表明TCR诱导的细胞凋亡涉及APO-1。我们在各种人类T细胞中验证了这一假设:(1)恶性Jurkat细胞,(2)同种异体反应性T细胞克隆(S13),以及(3)外周ATC。通过固定化抗CD3抗体或金黄色葡萄球菌肠毒素B(SEB)超抗原触发TCR可诱导这些细胞中APO-1配体的表达和细胞凋亡。即使在单细胞培养中也证实了抗CD3诱导的Jurkat细胞凋亡。在所有情况下,通过阻断抗APO-1抗体片段和可溶性APO-1受体诱饵,细胞凋亡均得到显著抑制。在活化的Jurkat细胞的上清液中发现APO-1配体是一种可溶性细胞因子。我们提出,ATC中TCR诱导的细胞凋亡可通过APO-1配体介导的自分泌自杀发生。这些结果为通过T细胞缺失抑制免疫反应和实现外周耐受提供了一种机制。
