Tsuyuguchi I
Osaka Prefectural Habikino Hospital, Japan.
Kekkaku. 1995 May;70(5):335-46.
One of the unique features characterizing human tuberculosis (TB) is its pathogenesis. The pathogenesis of TB involves cell-mediated immune responses against Mycobacterium tuberculosis. Concisely, macrophages activated by various soluble mediators or cytokines released through the cellular interactions after infection with M. tuberculosis play a pivotal role in the pathogenesis of human TB. In fact, very complex cellular interactions are going on within the host after infection with or endogenous reactivation of M. tuberculosis. Cells communicate by cell-cell contact and by the release of mediators which may originate locally, called cytokines. In TB infection, macrophages can be activated by two ways; directly with mycobacterial organisms or lipid fractions of their cell walls at the earlier phase of infection, and indirectly with cytokines produced by CD4+ T cells specifically activated by mycobacterial peptide antigens at the later phase of infection. The various clinical features of TB are the summarized outcome of cell to cell interactions mediated by diverse cytokines produced by various immune cells which are initially triggered by M. tuberculosis infection. CD4+ T cells can be classified into two subsets according to the patterns of cytokines they produce; Th1 cells give rise to cell-mediated immunity and are characterized by the production of IL-2 and IFN-gamma, whereas Th2 cells are more efficient in mediating antibody production and secrete IL-4, IL-5, IL-6 and IL-10. Th2 cells can control Th1 cells and vice versa. Th2 cells therefore inhibit the production of cytokines by Th1 cells by releasing IL-4 and IL-10. Infection with mycobacteria stimulates macrophage IL-12 production which appears to act directly on naive CD4+ T cells to induce Th1 development and initiation of cell-mediated immunity. IL-12 is a critical component in the development of cell-mediated immunity. In addition, IL-12 also activates NK cells and gamma/delta T cells, both of which secrete various macrophage-activating factors to kill M. tuberculosis. One of the structural characteristics of M. tuberculosis is the cell wall rich in lipid components. Of importance among various biological activities of the cell wall lipids is the stimulation of mononuclear phagocytes to produce a certain number of cytokines or monokines including IL-12 and IL-10, both of which play important roles in regulation of immune responses in mycobacterial infection and in pathogenesis of TB.(ABSTRACT TRUNCATED AT 400 WORDS)
人类结核病(TB)的一个独特特征是其发病机制。结核病的发病机制涉及针对结核分枝杆菌的细胞介导免疫反应。简而言之,在感染结核分枝杆菌后,通过细胞间相互作用释放的各种可溶性介质或细胞因子激活的巨噬细胞在人类结核病的发病机制中起关键作用。事实上,在感染结核分枝杆菌或其内源性再激活后,宿主体内会发生非常复杂的细胞间相互作用。细胞通过细胞间接触以及释放可能源自局部的介质(称为细胞因子)进行通讯。在结核病感染中,巨噬细胞可通过两种方式被激活;在感染早期直接与分枝杆菌生物体或其细胞壁的脂质部分接触,在感染后期间接与由分枝杆菌肽抗原特异性激活的CD4 + T细胞产生的细胞因子接触。结核病的各种临床特征是由结核分枝杆菌感染最初触发的各种免疫细胞产生的多种细胞因子介导的细胞间相互作用的总结结果。CD4 + T细胞可根据其产生的细胞因子模式分为两个亚群;Th1细胞引发细胞介导的免疫,其特征是产生IL-2和IFN-γ,而Th2细胞在介导抗体产生方面更有效,并分泌IL-4、IL-5、IL-6和IL-10。Th2细胞可以控制Th1细胞,反之亦然。因此,Th2细胞通过释放IL-4和IL-10抑制Th1细胞产生细胞因子。分枝杆菌感染刺激巨噬细胞产生IL-12,IL-12似乎直接作用于初始CD4 + T细胞以诱导Th1细胞发育并启动细胞介导的免疫。IL-12是细胞介导免疫发展的关键组成部分。此外,IL-12还激活NK细胞和γ/δT细胞,这两种细胞都会分泌各种巨噬细胞激活因子来杀死结核分枝杆菌。结核分枝杆菌的结构特征之一是其细胞壁富含脂质成分。在细胞壁脂质的各种生物学活性中,重要的是刺激单核吞噬细胞产生一定数量的细胞因子或单核因子,包括IL-12和IL-10,这两种因子在分枝杆菌感染的免疫反应调节和结核病发病机制中都发挥着重要作用。(摘要截取自400字)
