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Identification of Novel Biomarkers for Predicting Kidney Injury Due to Drugs Using “Omic” Strategies

机译:用“omic”策略为预测药物预测肾损伤的新型生物标志物

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Drug-induced kidney injury accounts for 20% of community- and hospital-acquired cases of acute kidney injury (AKI). The incidence is higher among older individuals, who often have co-existing morbidities and are exposed to more diagnostic procedures and therapies. While demographic and clinical components have been identified as risk factors, the proposed cellular mechanisms of drug-induced kidney injury are numerous and complicated. There are also limitations recognized in the use of traditional biomarkers, such as serum creatinine and blood urea nitrogen, to provide high sensitivity, specificity, and timeliness to identification of drug-induced kidney injury. Therefore, novel biomarkers are currently being investigated, identified, developed, and validated for their performance over the traditional biomarkers. This review will provide an overview of drug-induced kidney injury and will discuss what is known regarding "omic" (proteomic, genomic, transcriptomic, and metabolomic) biomarker strategies for drugs known to induce nephrotoxicity.? 2020 Awdishu et al.
机译:药物诱发的肾脏损伤占社区和医院获得的急性肾损伤(AKI)的20%。年龄较大的个体的发病率较高,他们经常具有共存的病症,并暴露于更多诊断程序和疗法。虽然人口统计和临床成分已被确定为危险因素,但提出的药物诱导的肾损伤的细胞机制无数并且复杂。在使用传统生物标志物(例如血清肌酐和血尿尿素氮)的使用中也有局限性识别,以提供高灵敏度,特异性和对鉴定药物诱导的肾损伤的良好性。因此,目前正在调查,确定,开发和验证新的生物标志物,以验证其对传统生物标志物的表现。本综述将概述药物诱导的肾损伤,并将讨论已知患有肾毒性的药物的“OMIC”(蛋白质组学,基因组,转录组和代谢组织)生物标志物策略的概述。 2020 AWDISHU等人。

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