Department of Immunology, Mayo Clinic, Rochester, MN 55905USA.
Graduate School of Biomedical Sciences, Mayo Clinic, Rochester, MN 55905USA.
Brain. 2024 Feb 1;147(2):566-589. doi: 10.1093/brain/awad319.
Cerebral malaria is the deadliest complication that can arise from Plasmodium infection. CD8 T-cell engagement of brain vasculature is a putative mechanism of neuropathology in cerebral malaria. To define contributions of brain endothelial cell major histocompatibility complex (MHC) class I antigen-presentation to CD8 T cells in establishing cerebral malaria pathology, we developed novel H-2Kb LoxP and H-2Db LoxP mice crossed with Cdh5-Cre mice to achieve targeted deletion of discrete class I molecules, specifically from brain endothelium. This strategy allowed us to avoid off-target effects on iron homeostasis and class I-like molecules, which are known to perturb Plasmodium infection. This is the first endothelial-specific ablation of individual class-I molecules enabling us to interrogate these molecular interactions. In these studies, we interrogated human and mouse transcriptomics data to compare antigen presentation capacity during cerebral malaria. Using the Plasmodium berghei ANKA model of experimental cerebral malaria (ECM), we observed that H-2Kb and H-2Db class I molecules regulate distinct patterns of disease onset, CD8 T-cell infiltration, targeted cell death and regional blood-brain barrier disruption. Strikingly, ablation of either molecule from brain endothelial cells resulted in reduced CD8 T-cell activation, attenuated T-cell interaction with brain vasculature, lessened targeted cell death, preserved blood-brain barrier integrity and prevention of ECM and the death of the animal. We were able to show that these events were brain-specific through the use of parabiosis and created the novel technique of dual small animal MRI to simultaneously scan conjoined parabionts during infection. These data demonstrate that interactions of CD8 T cells with discrete MHC class I molecules on brain endothelium differentially regulate development of ECM neuropathology. Therefore, targeting MHC class I interactions therapeutically may hold potential for treatment of cases of severe malaria.
脑型疟疾是由疟原虫感染引起的最致命的并发症。CD8 T 细胞与脑血管的相互作用是脑型疟疾神经病理学的一个假定机制。为了确定脑内皮细胞主要组织相容性复合体(MHC)I 类抗原呈递对 CD8 T 细胞在建立脑型疟疾病理中的作用,我们开发了新型 H-2Kb LoxP 和 H-2Db LoxP 小鼠,并与 Cdh5-Cre 小鼠杂交,以实现离散的 I 类分子的靶向缺失,特别是从脑内皮细胞中缺失。这种策略使我们能够避免对铁稳态和 I 类样分子的脱靶效应,这些分子已知会扰乱疟原虫感染。这是首次对单个 I 类分子进行内皮特异性消融,使我们能够研究这些分子间的相互作用。在这些研究中,我们分析了人类和小鼠的转录组学数据,以比较脑型疟疾期间的抗原呈递能力。使用伯氏疟原虫 ANKA 实验性脑型疟疾(ECM)模型,我们观察到 H-2Kb 和 H-2Db I 类分子调节不同的疾病发作模式、CD8 T 细胞浸润、靶向细胞死亡和区域性血脑屏障破坏。引人注目的是,从脑内皮细胞中缺失任何一种分子都会导致 CD8 T 细胞激活减少、T 细胞与脑血管的相互作用减弱、靶向细胞死亡减少、血脑屏障完整性得以保留,并预防 ECM 和动物死亡。我们通过使用联体共生和创建新型双小动物 MRI 技术来同时扫描感染期间的联体共生动物,证明了这些事件是脑特异性的。这些数据表明,CD8 T 细胞与脑内皮细胞离散 MHC I 类分子的相互作用可差异调节 ECM 神经病理学的发展。因此,针对 MHC I 类相互作用的治疗可能为严重疟疾的治疗提供潜在的治疗方法。
