Caforio A L, Bonifacio E, Keeling P J, Grazzini M, Schiaffino S, Bottazzo G F, McKenna W J
Department of Cardiological Sciences, St. George's Hospital Medical School, London, England.
G Ital Cardiol. 1992 Jan;22(1):63-72.
Aetiology and pathogenesis of idiopathic dilated cardiomyopathy (DCM) are uncertain. The two major pathogenetic hypotheses are: 1) autoimmunity; 2) persistent viral infection. Indirect evidence for virus association comes from the finding of raised titres of antibody to coxsackievirus in DCM, but infectious virus has never been isolated in myocardium from DCM patients. Bowles et al. using the slot-blotting technique reported that enteroviral RNA was commonly detectable in the myocardium of patients with myocarditis (53%) and with DCM (52%). Other groups using this as well as more refined hybridization techniques have failed to confirm such a high prevalence. Detection of enteroviral genomic RNA in cardiac tissue does not, however, imply active infection or pathogenicity. Thus the mechanisms of chronic myocardial damage in the absence of whole competent infectious virus remain uncertain. The other major pathogenetic hypothesis in DCM involves autoimmune mediated damage to myocytes. Circulating organ specific autoantibodies have been reported in a quarter of a group of patients with idiopathic DCM. This suggests that there may be autoimmune mechanisms operating at least in this subset of patients, but the exact relation of these antibodies to the pathogenesis and prognosis needs to be defined. The abnormal expression of major histocompatibility complex class II antigens on cardiac microvascular endothelium in endomyocardial biopsy tissue from DCM patients, and the reported association with HLA-DR4 phenotype lend further support to the autoimmune hypothesis. The viral and the autoimmune hypothesis in chronic myocarditis and in DCM are not mutually exclusive. In experimentally murine virus-induced myocarditis infectious virus can no longer be recovered from the myocardium after two weeks, although nucleic acid sequences of the viral genome are still detectable. The development of chronic inflammation takes place only in mice with a predisposing genetic background. Chronic myocyte damage is associated with the production of circulating heart-specific autoantibodies and autoreactive lymphocytes. In this animal model chronic myocarditis appears to be a virus-triggered or precipitated autoimmune disease, rather than a persistent viral infection with tissue damage due to active virus synthesis and replication. A similar transition from acute myocarditis into DCM may occur in man.
特发性扩张型心肌病(DCM)的病因和发病机制尚不清楚。两个主要的发病假说为:1)自身免疫;2)持续病毒感染。病毒关联的间接证据来自于在DCM患者中发现柯萨奇病毒抗体滴度升高,但从未在DCM患者的心肌中分离出感染性病毒。鲍尔斯等人使用狭缝印迹技术报告称,肠道病毒RNA在心肌炎患者(53%)和DCM患者(52%)的心肌中通常可检测到。其他使用该技术以及更精细杂交技术的研究小组未能证实如此高的患病率。然而,在心脏组织中检测到肠道病毒基因组RNA并不意味着存在活跃感染或致病性。因此,在没有完整活性感染性病毒的情况下,慢性心肌损伤的机制仍不确定。DCM的另一个主要发病假说涉及自身免疫介导的心肌细胞损伤。在一组特发性DCM患者中,四分之一的患者报告有循环器官特异性自身抗体。这表明至少在这部分患者中可能存在自身免疫机制,但这些抗体与发病机制和预后的确切关系需要明确。DCM患者心内膜活检组织中心脏微血管内皮细胞上主要组织相容性复合体II类抗原的异常表达,以及与HLA-DR4表型的报道关联,进一步支持了自身免疫假说。慢性心肌炎和DCM中的病毒假说和自身免疫假说并非相互排斥。在实验性小鼠病毒诱导的心肌炎中,两周后心肌中不再能回收感染性病毒,尽管病毒基因组的核酸序列仍可检测到。慢性炎症仅在具有易感遗传背景的小鼠中发生。慢性心肌细胞损伤与循环心脏特异性自身抗体和自身反应性淋巴细胞的产生有关。在这个动物模型中,慢性心肌炎似乎是一种病毒引发或促成的自身免疫性疾病,而不是由于活跃病毒合成和复制导致组织损伤的持续病毒感染。在人类中可能会发生类似的从急性心肌炎向DCM的转变。
