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首页> 外文期刊>Expert Review of Molecular Diagnostics >Biomarkers of drug-induced liver injury: progress and utility in research, medicine, and regulation
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Biomarkers of drug-induced liver injury: progress and utility in research, medicine, and regulation

机译:药物诱导肝损伤的生物标志物:研究,医学和监管中的进展和效用

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Introduction: The difficulty of understanding and diagnosing drug-induced liver injury (DILI) has led to proliferation of serum and genetic biomarkers. Many applications of these biomarkers have been proposed, including investigation of mechanisms, prediction of DILI during early trials or before initiation of therapy in patients, and diagnosis of DILI during therapy.Areas covered: We review the definition and categories of DILI, describe recent developments in DILI biomarker development, and provide guidance for future directions in DILI biomarker research. Expert commentary: There are major obstacles to DILI biomarker development and implementation, including the low prevalence of idiosyncratic DILI (IDILI), weak associations of IDILI with genetic variants, and lack of specificity of many biomarkers for the liver. Certain serum biomarkers, like miR-122, may have clinical utility in early-presenting patients with either intrinsic or idiosyncratic DILI in the future, while others likely will not find use. Future research should focus on implementation of biomarkers to predict later injury and outcome in early presenters with intrinsic DILI, and on development of biomarkers of adaptation and repair in the liver that can be used to determine if a liver test abnormality is likely to be clinically significant in IDILI.
机译:介绍:理解和诊断毒性肝损伤(DiRi)的难度导致了血清和遗传生物标志物的增殖。已经提出了许多这些生物标志物的应用,包括调查机制,早期试验期间的DIRI预测或在治疗患者的治疗前预测,以及治疗过程中的DILI诊断:我们审查了DILI的定义和类别,描述了最近的发展在帝力生物标志物的发展中,为Dili Biomarker Research的未来方向提供指导。专家评论:帝力生物标志物的开发和实施存在重大障碍,包括特质帝国帝力(idili)的低普遍率,偶然的遗传变异性缺乏关联,以及肝脏许多生物标志物的特异性。某些血清生物标志物,如miR-122,可能在早期呈现未来患有本质或特质的患者的临床效用,而其他人可能不会找到使用。未来的研究应该专注于实施生物标志物,以预测具有内在帝力的早期施用者的后期伤害和结果,以及可用于确定肝脏测试异常是否可能在临床上显着的肝脏的适应和修复生物标志物的发展在idili。

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