Department of Immunology, Wuhan University School of Medicine, Wuhan, People's Republic of China.
PLoS Pathog. 2010 May 20;6(5):e1000915. doi: 10.1371/journal.ppat.1000915.
The reports on the origin of human CD8(+) Valpha24(+) T-cell receptor (TCR) natural killer T (NKT) cells are controversial. The underlying mechanism that controls human CD4 versus CD8 NKT cell development is not well-characterized. In the present study, we have studied total 177 eligible patients and subjects including 128 healthy latent Epstein-Barr-virus(EBV)-infected subjects, 17 newly-onset acute infectious mononucleosis patients, 16 newly-diagnosed EBV-associated Hodgkin lymphoma patients, and 16 EBV-negative normal control subjects. We have established human-thymus/liver-SCID chimera, reaggregated thymic organ culture, and fetal thymic organ culture. We here show that the average frequency of total and CD8(+) NKT cells in PBMCs from 128 healthy latent EBV-infected subjects is significantly higher than in 17 acute EBV infectious mononucleosis patients, 16 EBV-associated Hodgkin lymphoma patients, and 16 EBV-negative normal control subjects. However, the frequency of total and CD8(+) NKT cells is remarkably increased in the acute EBV infectious mononucleosis patients at year 1 post-onset. EBV-challenge promotes CD8(+) NKT cell development in the thymus of human-thymus/liver-SCID chimeras. The frequency of total (3% of thymic cells) and CD8(+) NKT cells ( approximately 25% of NKT cells) is significantly increased in EBV-challenged chimeras, compared to those in the unchallenged chimeras (<0.01% of thymic cells, CD8(+) NKT cells undetectable, respectively). The EBV-induced increase in thymic NKT cells is also reflected in the periphery, where there is an increase in total and CD8(+) NKT cells in liver and peripheral blood in EBV-challenged chimeras. EBV-induced thymic CD8(+) NKT cells display an activated memory phenotype (CD69(+)CD45RO(hi)CD161(+)CD62L(lo)). After EBV-challenge, a proportion of NKT precursors diverges from DP thymocytes, develops and differentiates into mature CD8(+) NKT cells in thymus in EBV-challenged human-thymus/liver-SCID chimeras or reaggregated thymic organ cultures. Thymic antigen-presenting EBV-infected dendritic cells are required for this process. IL-7, produced mainly by thymic dendritic cells, is a major and essential factor for CD8(+) NKT cell differentiation in EBV-challenged human-thymus/liver-SCID chimeras and fetal thymic organ cultures. Additionally, these EBV-induced CD8(+) NKT cells produce remarkably more perforin than that in counterpart CD4(+) NKT cells, and predominately express CD8alphaalpha homodimer in their co-receptor. Thus, upon interaction with certain viruses, CD8 lineage-specific NKT cells are developed, differentiated and matured intrathymically, a finding with potential therapeutic importance against viral infections and tumors.
人类 CD8(+) Valpha24(+) T 细胞受体 (TCR) 自然杀伤 T (NKT) 细胞起源的报告存在争议。控制人类 CD4 与 CD8 NKT 细胞发育的潜在机制尚未很好地阐明。在本研究中,我们研究了总共 177 名合格的患者和受试者,包括 128 名健康潜伏 EBV 感染的受试者、17 名新发急性传染性单核细胞增多症患者、16 名新诊断的 EBV 相关霍奇金淋巴瘤患者和 16 名 EBV 阴性的正常对照受试者。我们建立了人胸腺/肝-SCID 嵌合体、重新聚集的胸腺器官培养和胎胸腺器官培养。我们在此表明,128 名健康潜伏 EBV 感染受试者的 PBMCs 中总 NKT 细胞和 CD8(+) NKT 细胞的平均频率明显高于 17 名急性 EBV 传染性单核细胞增多症患者、16 名 EBV 相关霍奇金淋巴瘤患者和 16 名 EBV 阴性正常对照受试者。然而,在急性 EBV 传染性单核细胞增多症患者发病后 1 年,总 NKT 细胞和 CD8(+) NKT 细胞的频率显著增加。EBV 刺激可促进人胸腺/肝-SCID 嵌合体中 CD8(+) NKT 细胞的发育。与未受 EBV 刺激的嵌合体相比,EBV 刺激的嵌合体中总 NKT 细胞(占胸腺细胞的 3%)和 CD8(+) NKT 细胞(约 NKT 细胞的 25%)的频率显著增加(分别为<0.01%的胸腺细胞,CD8(+) NKT 细胞不可检测)。EBV 诱导的胸腺 NKT 细胞增加也反映在周围组织中,在 EBV 刺激的嵌合体中,肝和外周血中的总 NKT 细胞和 CD8(+) NKT 细胞增加。EBV 诱导的胸腺 CD8(+) NKT 细胞显示出激活的记忆表型(CD69(+)CD45RO(hi)CD161(+)CD62L(lo))。在 EBV 刺激后,一部分 NKT 前体与 DP 胸腺细胞分离,在 EBV 刺激的人胸腺/肝-SCID 嵌合体或重新聚集的胸腺器官培养物中发育并分化为成熟的 CD8(+) NKT 细胞。胸腺中表达 EBV 的抗原呈递树突状细胞是这一过程所必需的。IL-7 主要由胸腺树突状细胞产生,是 EBV 刺激的人胸腺/肝-SCID 嵌合体和胎胸腺器官培养物中 CD8(+) NKT 细胞分化的主要和必需因子。此外,这些 EBV 诱导的 CD8(+) NKT 细胞产生的穿孔素明显多于相应的 CD4(+) NKT 细胞,并且在其共受体中主要表达 CD8alphaalpha 同源二聚体。因此,在与某些病毒相互作用时,CD8 谱系特异性 NKT 细胞在胸腺内发育、分化和成熟,这一发现对针对病毒感染和肿瘤具有潜在的治疗意义。
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