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脓毒症的生物标志物。

Biomarkers in sepsis.

机构信息

Centre for Heart Lung Innovation (HLI), St. Paul's Hospital, University of British Columbia, 1081 Burrard Street, Vancouver, BC, Canada, V6Z 1Y6,

出版信息

Curr Infect Dis Rep. 2013 Oct;15(5):413-20. doi: 10.1007/s11908-013-0357-x.

Abstract

There is much enthusiasm and interest in sepsis biomarkers, particularly because sepsis is a highly lethal condition, its diagnosis is challenging, and even simple treatment with antibiotics has led to serious adverse consequences such as emergence of resistant pathogens. Yet development of a sepsis biomarker requires many more steps than simply finding an association between a particular molecule and a clinical state or outcome. Demonstration of improvement of therapeutic practice using receiver-operating characteristic and other analyses is important. Validation in independent, prospective and, preferably, multicenter trials is essential. Many promising candidate sepsis biomarkers have recently been proposed. While procalcitonin (PCT) is currently the most studied sepsis biomarker, evidence of potential value has been found for a wide array of blood biomarkers including proteins, mRNA expression in whole blood or leukocytes, micro-RNAs (miRNA), pathogen and host DNA, pathogen and host genetic variants and metabolomic panels, and even in the novel use of currently available clinical data. While the most common early reports link putative sepsis biomarker levels to severity of illness and outcome (prognostic), this is not anticipated to be their primary use. More important is the distinction between infection and noninfectious inflammatory responses (diagnostic) and the use of sepsis biomarkers to direct therapy (predictive).

摘要

人们对脓毒症生物标志物非常感兴趣,特别是因为脓毒症是一种高死亡率的疾病,其诊断具有挑战性,即使是简单的抗生素治疗也会导致严重的不良后果,如耐药病原体的出现。然而,开发脓毒症生物标志物需要比简单地发现特定分子与临床状态或结果之间的关联更多的步骤。使用接收者操作特征和其他分析来证明治疗实践的改善是很重要的。在独立的、前瞻性的、最好是多中心的试验中进行验证是必不可少的。最近提出了许多有前途的候选脓毒症生物标志物。虽然降钙素原(PCT)是目前研究最多的脓毒症生物标志物,但在广泛的血液生物标志物中也发现了有潜在价值的证据,包括蛋白质、全血或白细胞中的 mRNA 表达、微小 RNA(miRNA)、病原体和宿主 DNA、病原体和宿主遗传变异以及代谢组学图谱,甚至在目前可用的临床数据的新用途上。虽然最常见的早期报告将推测的脓毒症生物标志物水平与疾病严重程度和预后(预后)联系起来,但预计这不是它们的主要用途。更重要的是区分感染和非感染性炎症反应(诊断)以及使用脓毒症生物标志物来指导治疗(预测)。

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