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Classification and histological, immunohistochemical, and molecular diagnosis of inflammatory myocardial disease

机译:炎性心肌病的分类和组织学,免疫组化和分子诊断

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In the WHO 1996 classification of cardiomyopathies, myocarditis is defined as an "inflammatory disease of the myocardium associated with cardiac dysfunction" and is listed among "specific cardiomyopathies". Myocarditis is diagnosed on endomyocardial biopsy (EMB) by established histological, immunological, and immunohistochemical criteria, and molecular techniques are recommended to identify viral etiology. Infectious, autoimmune, and idiopathic forms of inflammatory cardiomyopathy are recognized that may lead to dilated cardiomyopathy. According to Dallas criteria, myocarditis is diagnosed in the setting of an "inflammatory infiltrate of the myocardium with necrosis and/or degeneration of adjacent myocytes, not typical of ischemic damage associated with coronary artery disease". The majority of experts in the field agree that an actual increase in sensitivity of EMB has now been reached by using immunohistochemistry together with histology. A value of 14 leukocytes/mm2 with the presence of T lymphocytes 7 cells/mm2 has been considered a realistic cut off to reach a diagnosis of myocarditis. The development of molecular biological techniques, particularly amplification methods like polymerase chain reaction (PCR) or nested-PCR, allows the detection of low copy viral genomes even from an extremely small amount of tissue such as in EMB specimens. Positive PCR results obtained on EMB should always be accompanied by a parallel investigation on blood samples collected at the time of the EMB. According to the recent Association for European Cardiovascular Pathology guidelines, optimal specimen procurement and triage indicates at least three, preferably four, EMB fragments, each 1-2 mm in size, that should immediately be fixed in 10 % buffered formalin at room temperature for light microscopic examination. In expected focal myocardial lesions, additional sampling is recommended. Moreover, one or two specimens should be snap-frozen in liquid nitrogen and stored at -80 C or alternatively stored in RNA-later for possible molecular tests or specific stains. A sample of peripheral blood (5-10 ml) in EDTA or citrate from patients with suspected myocarditis allows molecular testing for the same viral genomes sought in the myocardial tissue.
机译:在WHO 1996的心肌病分类中,心肌炎被定义为“与心脏功能障碍有关的心肌炎性疾病”,并被列为“特定的心肌病”。根据已建立的组织学,免疫学和免疫组织化学标准,可通过心内膜活检(EMB)诊断出心肌炎,并建议使用分子技术来鉴定病毒病因。感染性,自身免疫性和特发性形式的炎症性心肌病被认为可能导致扩张型心肌病。根据达拉斯标准,心肌炎被诊断为“心肌炎性浸润伴邻近细胞坏死和/或变性,不是与冠状动脉疾病相关的缺血性损害的典型表现”。该领域的大多数专家都认为,通过使用免疫组织化学和组织学,现已达到了EMB敏感性的实际提高。 T淋巴细胞> 7细胞/ mm2时,> 14白细胞/ mm2的值被认为是达到诊断心肌炎的现实的标准。分子生物学技术的发展,特别是诸如聚合酶链反应(PCR)或巢式PCR之类的扩增方法,甚至可以从极少量的组织(例如EMB标本)中检测低拷贝病毒基因组。在EMB上获得阳性PCR结果时,应始终并行进行EMB采集时的血样调查。根据最近的欧洲心血管病理学协会指南,最佳的标本采集和分类表明,至少有三个,最好是四个EMB片段,每个1-2毫米大小,应立即在室温下固定在10%福尔马林缓冲液中以避光显微镜检查。在预期的局灶性心肌病变中,建议额外取样。此外,应将一两个样本在液氮中速冻,并在-80℃下保存,或在后来的RNA中保存,以进行可能的分子检测或特定的染色。从疑似心肌炎患者的EDTA或柠檬酸盐中提取外周血(5-10毫升),可以对心肌组织中寻求的相同病毒基因组进行分子检测。

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