Soos J M, Hobeika A C, Butfiloski E J, Schiffenbauer J, Johnson H M
Department of Microbiology and Cell Science, University of Florida, Gainesville 32611, USA.
Proc Natl Acad Sci U S A. 1995 Jun 20;92(13):6082-6. doi: 10.1073/pnas.92.13.6082.
Superantigens such as the staphylococcal enterotoxins can play an important role in exacerbation of autoimmune disorders such as experimental allergic encephalomyelitis (EAE) in mice. In fact, superantigens can reactivate EAE in PL/J mice that have been sensitized to rat myelin basic protein (MBP). The T-cell subset predominantly responsible for disease in PL/J mice bears the V beta 8+ T-cell antigen receptor (TCR). The question arises as to whether T cells bearing other V beta specificities are involved in induction or reactivation of EAE with superantigen. Thus, we have investigated the ability of a non-V beta 8-specific superantigen, staphylococcal enterotoxin A (SEA) (V beta specificities 1, 3, 10, 11, and 17), to induce EAE in PL/J mice that have been previously protected from disease by anergy and deletion of V beta 8+ T cells. PL/J mice were first pretreated with the V beta 8-specific superantigen staphylococcal enterotoxin B (SEB) and then immunized with MBP. These mice exhibited V beta 8-specific anergy and depletion and did not develop EAE, even when further treated with SEB. However, administration of SEA to these same mice induced an initial episode of EAE which was characterized by severe hindleg paralysis and accelerated onset of disease. In contrast to SEB pretreatment, PL/J mice pretreated with SEA did develop EAE when immunized with MBP, and after resolution of clinical signs of disease these mice were susceptible to relapse of EAE induced by SEB but not by SEA. Thus, superantigens can activate encephalitogenic MBP-specific non-V beta 8+ T cells to cause EAE in PL/J mice. These data suggest that superantigens can play a central role in autoimmune disorders and that they introduce a profound complexity to autoimmune diseases such as EAE, akin to the complexity seen in multiple sclerosis.
诸如葡萄球菌肠毒素之类的超抗原在加重自身免疫性疾病(如小鼠实验性变应性脑脊髓炎,EAE)中可发挥重要作用。事实上,超抗原可使已对大鼠髓鞘碱性蛋白(MBP)致敏的PL/J小鼠体内的EAE重新激活。在PL/J小鼠中,主要导致疾病的T细胞亚群带有Vβ8 + T细胞抗原受体(TCR)。于是就产生了一个问题,即带有其他Vβ特异性的T细胞是否参与了超抗原诱导或重新激活EAE的过程。因此,我们研究了一种非Vβ8特异性超抗原——葡萄球菌肠毒素A(SEA)(Vβ特异性为1、3、10、11和17)在曾因Vβ8 + T细胞失能和缺失而免受疾病影响的PL/J小鼠中诱导EAE的能力。PL/J小鼠首先用Vβ8特异性超抗原葡萄球菌肠毒素B(SEB)进行预处理,然后用MBP免疫。这些小鼠表现出Vβ8特异性失能和耗竭,即使再次用SEB处理也不会发生EAE。然而,给这些相同的小鼠施用SEA会诱导EAE的初次发作,其特征为严重的后肢麻痹和疾病快速发作。与SEB预处理不同,用SEA预处理的PL/J小鼠在用MBP免疫时确实发生了EAE,并且在疾病临床症状消退后,这些小鼠易受SEB诱导的EAE复发影响,但不受SEA诱导的EAE复发影响。因此,超抗原可激活致脑炎性MBP特异性非Vβ8 + T细胞,从而在PL/J小鼠中引发EAE。这些数据表明,超抗原在自身免疫性疾病中可发挥核心作用,并且它们给诸如EAE之类的自身免疫性疾病带来了极大的复杂性,类似于在多发性硬化症中所见的复杂性。