Prinz Marco, Garbe Folker, Schmidt Hauke, Mildner Alexander, Gutcher Ilona, Wolter Karina, Piesche Matthias, Schroers Roland, Weiss Elisabeth, Kirschning Carsten J, Rochford Christian D P, Brück Wolfgang, Becher Burkhard
Institute of Neuropathology, Georg-August-University, Gottingen, Germany.
J Clin Invest. 2006 Feb;116(2):456-64. doi: 10.1172/JCI26078. Epub 2006 Jan 26.
Inflammatory diseases of the CNS, such as MS and its animal model EAE, are characterized by infiltration of activated lymphocytes and phagocytes into the CNS. Within the CNS, activation of resident cells initiates an inflammatory cascade, leading to tissue destruction, demyelination, and neurologic deficit. TLRs recognize microbes and are pivotal mediators of innate immunity. Within the CNS, augmented TLR expression during EAE is observed, even in the absence of any apparent microbial involvement. To determine the functional relevance of this phenomenon during sterile autoimmunity, we studied the role of different TLRs as well as their common signaling adaptor MyD88 in the development of EAE. We found that MyD88 mice were completely EAE resistant. Surprisingly, this protection is partly due to engagement of the CpG receptor TLR9. Restricting the MyD88 or TLR9 mutation to host radio-resistant cells, including the cells within the CNS, revealed that engagement of radio-resistant cells modulated the disease course and histopathological changes. Our data clearly demonstrate that both TLR9 and MyD88 are essential modulators of the autoimmune process during the effector phase of disease and suggest that endogenous "danger signals" modulate the disease pathogenesis.
中枢神经系统的炎症性疾病,如多发性硬化症及其动物模型实验性自身免疫性脑脊髓炎(EAE),其特征是活化的淋巴细胞和吞噬细胞浸润到中枢神经系统。在中枢神经系统内,驻留细胞的活化引发炎症级联反应,导致组织破坏、脱髓鞘和神经功能缺损。Toll样受体(TLRs)识别微生物,是固有免疫的关键介质。在中枢神经系统内,即使在没有任何明显微生物参与的情况下,EAE期间也观察到TLR表达增加。为了确定这种现象在无菌自身免疫过程中的功能相关性,我们研究了不同TLRs及其共同信号转导衔接蛋白髓样分化因子88(MyD88)在EAE发病过程中的作用。我们发现MyD88基因敲除小鼠对EAE完全具有抗性。令人惊讶的是,这种保护作用部分归因于CpG受体TLR9的参与。将MyD88或TLR9突变限制在宿主抗辐射细胞(包括中枢神经系统内的细胞)中,结果表明抗辐射细胞的参与调节了疾病进程和组织病理学变化。我们的数据清楚地表明,TLR9和MyD88在疾病效应阶段都是自身免疫过程的重要调节因子,并提示内源性“危险信号”调节疾病发病机制。