Henke A, Huber S, Stelzner A, Whitton J L
Department of Neuropharmacology, Scripps Research Institute, La Jolla, California 92037, USA.
J Virol. 1995 Nov;69(11):6720-8. doi: 10.1128/JVI.69.11.6720-6728.1995.
Coxsackievirus infections have previously been shown to cause acute or chronic myocarditis in humans, and several mouse models have been established to study the pathology of this disease. Myocardial injury may result from direct viral effects and/or may be immune mediated. To determine the relative roles of these processes in pathogenesis, we have compared coxsackievirus B3 (CVB3) infections of normal and immuno-compromised transgenic knockout (ko) mice. CVB3 was able to infect all strains used (C57BL/6, CD4ko, and beta-microglobulin ko [beta 2Mko]), and following intraperitoneal injection, two disease processes could be distinguished. First, the virus caused early (3 to 7 days postinfection) death in a viral dose-dependent manner. Immunocompetent C57BL/6 mice were highly susceptible (50% lethal dose = 70 PFU), while immunodeficient transgenic ko mice were less susceptible, showing 10- and 180-fold increases in the 50% lethal dose (for CD4ko and beta 2Mko mice, respectively). Second, a histologic examination of surviving CD4ko mice at 7 days postinfection revealed severe myocarditis; the inflammatory infiltrate comprised 40 to 50% macrophages, 30 to 40% NK cells, and 10 to 20% CD8+ T lymphocytes. The infiltration resolved over the following 2 to 3 weeks, with resultant myocardial fibrosis. In vivo depletion of CD8+ T lymphocytes from these CD4ko mice led to a marked reduction in myocarditis and an increase in myocardial virus titers. beta 2Mko mice, which lack antiviral CD8+ T cells, are much less susceptible to early death and to the development of myocarditis. We conclude that our data support a strong immunopathologic component in CVB3-induced disease and implicate both CD4+ and CD8+ T cells. Compared with immunocompetent animals, (i) mice lacking CD4+ T cells (CD4ko) were more resistant to virus challenge, and (ii) mice lacking CD8+ T cells (beta 2Mko and in vivo-depleted CD4ko) showed enhanced survival and a reduced incidence of the later myocarditis. Nevertheless, the picture is complex, since (iii) removal of the CD4+ component, while protecting against early death, greatly magnified the severity of myocarditis, and (iv) removal of the CD8+ cells from CD4ko mice, although protecting against early death and later myocarditis, led to markedly increased virus titers in the heart. These data underscore the complex balance between the costs and benefits of effective antiviral immune responses.
先前已证明柯萨奇病毒感染可导致人类急性或慢性心肌炎,并且已经建立了几种小鼠模型来研究这种疾病的病理学。心肌损伤可能是由病毒的直接作用引起的和/或可能是免疫介导的。为了确定这些过程在发病机制中的相对作用,我们比较了正常和免疫受损的转基因敲除(ko)小鼠的柯萨奇病毒B3(CVB3)感染情况。CVB3能够感染所有使用的品系(C57BL/6、CD4ko和β2微球蛋白ko [β2Mko]),腹腔注射后,可以区分出两种疾病过程。首先,病毒以病毒剂量依赖性方式导致早期(感染后3至7天)死亡。免疫健全的C57BL/6小鼠高度易感(半数致死剂量 = 70 PFU),而免疫缺陷的转基因ko小鼠较不易感,其半数致死剂量分别增加了10倍和180倍(分别针对CD4ko和β2Mko小鼠)。其次,对感染后7天存活的CD4ko小鼠进行组织学检查发现严重心肌炎;炎性浸润包括40%至50%的巨噬细胞、30%至40%的自然杀伤细胞和10%至20%的CD8+ T淋巴细胞。浸润在接下来的2至3周内消退,导致心肌纤维化。从这些CD4ko小鼠体内清除CD8+ T淋巴细胞导致心肌炎明显减轻,心肌病毒滴度增加。缺乏抗病毒CD8+ T细胞的β2Mko小鼠对早期死亡和心肌炎的发生更不易感。我们得出结论,我们的数据支持CVB3诱导疾病中存在强大的免疫病理成分,并涉及CD4+和CD8+ T细胞。与免疫健全的动物相比,(i)缺乏CD4+ T细胞(CD4ko)的小鼠对病毒攻击更具抵抗力,并且(ii)缺乏CD8+ T细胞(β2Mko和体内清除CD4+的CD4ko)的小鼠存活率提高,后期心肌炎的发病率降低。然而,情况很复杂,因为(iii)去除CD4+成分虽然能预防早期死亡,但大大放大了心肌炎的严重程度,并且(iv)从CD4ko小鼠中去除CD8+细胞,虽然能预防早期死亡和后期心肌炎,但导致心脏中的病毒滴度明显增加。这些数据强调了有效的抗病毒免疫反应的成本和益处之间的复杂平衡。
