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首页> 外文期刊>Regulatory Toxicology and Pharmacology: RTP >Enhancing the utility of alanine aminotransferase as a reference standard biomarker for drug-induced liver injury
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Enhancing the utility of alanine aminotransferase as a reference standard biomarker for drug-induced liver injury

机译:增强丙氨酸氨基转移酶作为药物诱导肝损伤的参考标准生物标志物的效用

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摘要

Drug-induced liver injury (DILI) is the most frequent cause of discontinuation of new chemical entities during development. DILI can either be intrinsic/predictable or an idiosyncratic type. These two forms of DILI are contrasted in their manifestation and diagnosis. Even with regulatory guidance (FDA, 2009), there is still a gap in our ability to identify predictable DILI, both specifically and sensitively. Alanine aminotransferase (ALT) is the principal reference standard biomarker to diagnose DILI, yet its current application in preclinical to clinical translation for decision-making purposes has imperfections: (1) analytical ALT assay uniformity across industry would be aided by common analytical processes; (2) assessment of ALT toxicological performance in a large preclinical analysis would help to establish a true threshold of elevation for predictable DILI and improve translational use across various stages of pharmaceutical development and finally, (3) clinical evaluation of ALT elevations prospectively and retrospectively is recommended to define and manage variations in clinical study subjects including rising body mass index (BMI) range and ALT upper limit of normal (ULN) in the broader population over time. The emergence of new hepatotoxicity biomarkers necessitates a parallel and equivalent assessment to the aminotrans-ferases in a regulatory qualification model.
机译:药物诱导的肝损伤(DILI)是在发育过程中排除新化学实体的最常见原因。帝力可以是内在/可预测的或特殊类型。这两种形式的Dili在其表现和诊断中形成鲜明对比。即使采用监管指导(FDA,2009),我们仍然有能力识别可预测的帝力,特别是敏感的能力。丙氨酸氨基转移酶(ALT)是诊断DILI的主要参考标准生物标志物,但其目前在临床前应用于决策目的的临床翻译,具有缺陷:(1)跨行业的分析施工均匀性将通过常见的分析过程辅助。 (2)评估ALT毒理学性能在大型临床前分析将有助于为可预测的DILI建立真正的升高阈值,并改善了在药物发育的各个阶段的平移使用,最后,前瞻性和回顾性临床评价ALT海拔建议在更广泛的人口中定义和管理临床研究受试者的变化,包括身体质量指数(BMI)范围和正常(ULN)的ALT上限。新的肝毒性生物标志物的出现需要对监管鉴定模型中的氨管 - 氨基胺进行平行和等同的评估。

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