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早期心肌缺血的分子组织变化:从病理生理学到新诊断标志物的识别

Molecular tissue changes in early myocardial ischemia: from pathophysiology to the identification of new diagnostic markers.

作者信息

Aljakna Aleksandra, Fracasso Tony, Sabatasso Sara

机构信息

University Center of Legal Medicine Lausanne-Geneva (CURML), Rue Michel-Servet 1, 1211, Geneva, Switzerland.

出版信息

Int J Legal Med. 2018 Mar;132(2):425-438. doi: 10.1007/s00414-017-1750-z. Epub 2018 Jan 23.

Abstract

Diagnosing early myocardial ischemia (the initial 4 to 6 h after interruption of blood flow to part of the myocardium) remains a challenge for clinical and forensic pathologists. Several immunohistochemical markers have been proposed for improving postmortem detection of early myocardial ischemia; however, no single marker appears to be both sufficiently specific as well as sensitive. This review summarizes the diverse categories of molecular tissue markers that have been investigated in human autopsy samples with acute myocardial infarction as well as in the well-established and widely used in vivo animal model of early myocardial ischemia (permanent ligation of the coronary artery). Recently identified markers appearing during the initial 2 h of myocardial ischemia are highlighted. Among them, only six were tested for specificity (C5b-9, hypoxia-inducible factor 1-alpha, vascular endothelial growth factor, heart fatty acid binding protein, connexin 43, and JunB). Despite the discovery of several potentially promising markers (in terms of early expression and specificity), many of them remain to be tested and validated for application in routine diagnostics in clinical and forensic pathology. In particular, research investigating the postmortem stability of these markers is required before any might be implemented into routine diagnostics. Establishing a standardized panel of immunohistochemical markers may be more useful for improving sensitivity and specificity than searching for a single marker.

摘要

诊断早期心肌缺血(心肌部分血流中断后的最初4至6小时)对临床病理学家和法医病理学家来说仍是一项挑战。已经提出了几种免疫组化标志物以改善早期心肌缺血的死后检测;然而,似乎没有单一标志物既具有足够的特异性又具有足够的敏感性。本综述总结了在急性心肌梗死人体尸检样本以及成熟且广泛使用的早期心肌缺血体内动物模型(冠状动脉永久性结扎)中研究的多种分子组织标志物类别。重点介绍了在心肌缺血最初2小时内出现的最近鉴定出的标志物。其中,仅对六种标志物进行了特异性测试(C5b-9、缺氧诱导因子1-α、血管内皮生长因子、心脏脂肪酸结合蛋白、连接蛋白43和JunB)。尽管发现了几种潜在有前景的标志物(就早期表达和特异性而言),但其中许多仍有待在临床和法医病理学的常规诊断中进行测试和验证。特别是,在将这些标志物应用于常规诊断之前,需要研究它们的死后稳定性。建立标准化的免疫组化标志物组合可能比寻找单一标志物更有助于提高敏感性和特异性。

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