Renno T, Krakowski M, Piccirillo C, Lin J Y, Owens T
Montreal Neurological Institute, Quebec, Canada.
J Immunol. 1995 Jan 15;154(2):944-53.
The inflammatory cytokines IFN-gamma and TNF-alpha have been demonstrated in various autoimmune diseases, and are thought to participate in the induction and pathogenesis of disease. TFN-alpha is a cytopathic cytokine that is cytotoxic for oligodendrocytes in vitro and has been implicated in the pathology of multiple sclerosis and its animal model experimental allergic encephalomyelitis (EAE). We used reverse transcriptase (RT)-PCR to study the kinetics, cellular source, and regulation of cytokine gene expression in the central nervous system (CNS) of SJL/J mice with myelin basic protein-induced EAE at different stages of the disease. The expression of CD3, IL-2, IFN-gamma, and TNF-alpha mRNA was barely detectable in the CNS of unmanipulated mice or mice that were immunized with adjuvant but showed no symptoms. These mRNAs were readily detectable in the CNS of mice during peak disease, then coordinately dropped to background levels during remission. Analysis of cells isolated from the CNS of mice with acute EAE showed that the Th1 cytokines, IL-2 and IFN-gamma, were produced by infiltrating CD4+ T cells. In contrast, TNF-alpha was predominantly transcribed by non-T mononuclear CNS cells, the majority of which were identified as microglia and macrophages by their Mac-1 phenotype. Microglia could be discriminated by their low expression of CD45. Incubation of freshly derived, adult microglia from normal, uninfiltrated, CNS with activated Th1 supernatant induced the production of TNF-alpha mRNA. Therefore, TNF-alpha is made by both CNS-resident microglia and infiltrating macrophages during EAE, and this production is tightly controlled by cytokines secreted by infiltrating CD4+ T cells.
炎症细胞因子γ干扰素(IFN-γ)和肿瘤坏死因子-α(TNF-α)已在多种自身免疫性疾病中得到证实,并被认为参与了疾病的诱导和发病机制。TNF-α是一种细胞病变性细胞因子,在体外对少突胶质细胞具有细胞毒性,并与多发性硬化症及其动物模型实验性变应性脑脊髓炎(EAE)的病理过程有关。我们使用逆转录酶(RT)-PCR研究了髓鞘碱性蛋白诱导的EAE不同阶段的SJL/J小鼠中枢神经系统(CNS)中细胞因子基因表达的动力学、细胞来源和调控。在未处理的小鼠或用佐剂免疫但无症状的小鼠的CNS中,几乎检测不到CD3、白细胞介素-2(IL-2)、IFN-γ和TNF-α mRNA的表达。在疾病高峰期,这些mRNA在小鼠的CNS中很容易检测到,然后在缓解期协同下降到背景水平。对急性EAE小鼠CNS分离的细胞分析表明,Th1细胞因子IL-2和IFN-γ由浸润的CD4+ T细胞产生。相比之下,TNF-α主要由非T单核CNS细胞转录,其中大多数通过其Mac-1表型被鉴定为小胶质细胞和巨噬细胞。小胶质细胞可通过其低表达的CD45来区分。用活化的Th1上清液孵育来自正常、未浸润的CNS的新鲜分离的成年小胶质细胞,可诱导TNF-α mRNA的产生。因此,在EAE期间,TNF-α由CNS驻留的小胶质细胞和浸润的巨噬细胞产生,并且这种产生受到浸润的CD4+ T细胞分泌的细胞因子的严格控制。
