Department of Immunology and.
Department of Comparative Medicine, University of Washington, Seattle, Washington, USA.
J Clin Invest. 2020 Jan 2;130(1):203-213. doi: 10.1172/JCI132531.
Multiple sclerosis (MS) is an inflammatory, demyelinating disease of the CNS. Although CD4+ T cells are implicated in MS pathogenesis and have been the main focus of MS research using the animal model experimental autoimmune encephalomyelitis (EAE), substantial evidence from patients with MS points to a role for CD8+ T cells in disease pathogenesis. We previously showed that an MHC class I-restricted epitope of myelin basic protein (MBP) is presented in the CNS during CD4+ T cell-initiated EAE. Here, we investigated whether naive MBP-specific CD8+ T cells recruited to the CNS during CD4+ T cell-initiated EAE engaged in determinant spreading and influenced disease. We found that the MBP-specific CD8+ T cells exacerbated brain but not spinal cord inflammation. We show that a higher frequency of monocytes and monocyte-derived cells presented the MHC class I-restricted MBP ligand in the brain compared with the spinal cord. Infiltration of MBP-specific CD8+ T cells enhanced ROS production in the brain only in these cell types and only when the MBP-specific CD8+ T cells expressed Fas ligand (FasL). These results suggest that myelin-specific CD8+ T cells may contribute to disease pathogenesis via a FasL-dependent mechanism that preferentially promotes lesion formation in the brain.
多发性硬化症(MS)是一种中枢神经系统的炎症性脱髓鞘疾病。虽然 CD4+T 细胞被认为与 MS 的发病机制有关,并且一直是使用动物模型实验性自身免疫性脑脊髓炎(EAE)进行 MS 研究的主要焦点,但来自 MS 患者的大量证据表明 CD8+T 细胞在疾病发病机制中起作用。我们之前曾表明,髓鞘碱性蛋白(MBP)的 MHC Ⅰ类限制性表位在 CD4+T 细胞引发的 EAE 期间在中枢神经系统中呈现。在这里,我们研究了在 CD4+T 细胞引发的 EAE 期间募集到中枢神经系统的幼稚 MBP 特异性 CD8+T 细胞是否参与了决定簇扩展并影响疾病。我们发现 MBP 特异性 CD8+T 细胞加剧了大脑而非脊髓的炎症。我们表明,与脊髓相比,大脑中呈现 MHC Ⅰ类限制性 MBP 配体的单核细胞和单核细胞衍生细胞的频率更高。仅在这些细胞类型中,并且仅当 MBP 特异性 CD8+T 细胞表达 Fas 配体(FasL)时,MBP 特异性 CD8+T 细胞的浸润才会增加大脑中的 ROS 产生。这些结果表明,髓鞘特异性 CD8+T 细胞可能通过 FasL 依赖性机制促进疾病发病机制,该机制优先促进大脑中的病变形成。
