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Development of blood biomarkers for drug-induced liver injury: An evaluation of their potential for risk assessment and diagnostics

机译:药物性肝损伤的血液生物标志物的开发:对其风险评估和诊断潜力的评估

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摘要

Drug-induced liver injury (DILI) remains a rare but serious complication in drug therapy that is a primary cause of drug failure during clinical trials. Conventional biomarkers, particularly the serum transaminases and bilirubin, serve as useful indicators of hepatocellular or cholestatic liver injury, respectively, but only after substantial and sometimes irreversible tissue damage. Ideally, more sensitive biomarkers that respond very early before irreversible injury has occurred would offer improved outcomes. Novel biomarkers are initially being developed in animal models exposed to intrinsically hepatotoxic stimuli. However, the eventual translation to human populations, even those with known risk factors that predispose the liver to drug toxicity, would be the fundamental goal. Ultimately, some might even be applicable for the early identification of individuals predisposed to idiosyncratic hepatotoxicity potential. This article reviews recent progress in the discovery and qualification of novel biomarkers for DILI and delineates the path to eventual utilization for risk assessment. Some major categories of plasma or serum biomarkers surveyed include proteins, cytokines, circulating mRNAs, and microRNAs.
机译:药物诱发的肝损伤(DILI)在药物治疗中仍然是一种罕见但严重的并发症,是临床试验期间药物衰竭的主要原因。常规的生物标志物,特别是血清转氨酶和胆红素,分别作为肝细胞或胆汁淤积性肝损伤的有用指示剂,但仅在实质性且有时是不可逆转的组织损伤后才起作用。理想地,在不可逆损伤发生之前很早就做出反应的更敏感的生物标志物将提供更好的结果。新型生物标志物最初是在暴露于固有肝毒性刺激的动物模型中开发的。但是,最终的目标人群是最终的目标人群,即使是那些具有已知危险因素的人群也可能使肝脏对药物产生毒性。最终,有些甚至可能适用于早期识别易特发性肝毒性的个体。本文回顾了DILI新型生物标志物发现和鉴定的最新进展,并勾勒了最终用于风险评估的途径。所调查的血浆或血清生物标志物的一些主要类别包括蛋白质,细胞因子,循环mRNA和microRNA。

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