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炎症性和非炎症性心肌病中的生物标志物。

Biomarkers in inflammatory and noninflammatory cardiomyopathy.

作者信息

Noutsias Michel, Pankuweit Sabine, Maisch Bernhard

机构信息

Department of Internal Medicine - Cardiology, University Hospital of Marburg and Giessen/UKGM GmbH, Faculty of Medicine, Philipps University of Marburg, Marburg, Germany.

出版信息

Herz. 2009 Dec;34(8):614-23. doi: 10.1007/s00059-009-3318-2.

Abstract

Acute myocarditis (AMC) and its sequela, dilated cardiomyopathy (DCM), are most often caused by cardiotropic viral infections in the Western world. Inflammatory cardiomyopathy (DCMi) is a specific cardiomyopathy entity of DCM, being defined by the proof of intramyocardial inflammation and/or viral infection in endomyocardial biopsies (EMBs). Diagnostic procedures of EMBs are indispensable for the etiopathogenic differentiation of the disease. Experienced cardiology centers have reported low complication rates of EMB obtainment. The histological Dallas criteria are prone to substantial sampling error and interobserver variability, have no prognostic impact and, moreover, are not suitable to select AMC/DCMi patients who favorably respond to immunosuppression. Immunohistological detection of myocarditis and viral persistence have proven adverse prognostic impact in AMC and DCM patients, respectively. This contemporary diagnostic repertoire on EMBs is essential for the selection of DCMi patients who will likely benefit from immunomodulatory treatment, which has been addressed in randomized trials. During the past decade, cardiac magnetic resonance (CMR) has developed as a valuable noninvasive diagnostic approach for the detection and localization of intramyocardial inflammation, and CMR guidelines for AMC have been elaborated. Late gadolinium enhancement (LGE) has been associated with adverse prognostic outcome in DCM patients. CMR techniques, however, are not suitable to specifically detect myocardial viral infections. To date, no classic biomarker has been shown to differentiate between DCMi and noninflammatory cardiomyopathies.

摘要

在西方世界,急性心肌炎(AMC)及其后遗症扩张型心肌病(DCM)最常由嗜心性病毒感染引起。炎症性心肌病(DCMi)是DCM的一种特定心肌病实体,通过心内膜心肌活检(EMB)中存在心肌内炎症和/或病毒感染来定义。EMB的诊断程序对于该疾病的病因学鉴别不可或缺。经验丰富的心脏病学中心报告称EMB获取的并发症发生率较低。组织学达拉斯标准容易出现大量抽样误差和观察者间差异,对预后没有影响,而且不适用于选择对免疫抑制有良好反应的AMC/DCMi患者。心肌炎的免疫组织学检测和病毒持续存在已分别在AMC和DCM患者中被证明具有不良预后影响。这种关于EMB的当代诊断方法对于选择可能从免疫调节治疗中获益的DCMi患者至关重要,这一点已在随机试验中得到探讨。在过去十年中,心脏磁共振成像(CMR)已发展成为一种用于检测和定位心肌内炎症的有价值的非侵入性诊断方法,并且已经制定了AMC的CMR指南。延迟钆增强(LGE)与DCM患者的不良预后相关。然而,CMR技术并不适合特异性检测心肌病毒感染。迄今为止,尚未发现经典生物标志物能够区分DCMi和非炎症性心肌病。

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