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Diagnosis of Acute Kidney Injury Using Functional and Injury Biomarkers: Workgroup Statements from the Tenth Acute Dialysis Quality Initiative Consensus Conference

机译:使用功能和损伤生物标志物的诊断急性肾损伤:第十个急性透析质量倡议协商会议的工作组陈述

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Acute kidney injury (AKI) commonly occurs in hospitalized patients and is independently and strongly associates with morbidity and mortality. The clinical benefits of a timely and definitive diagnosis of AKI have not been fully realized due to limitations imposed by the use of serum creatinine and urine outputto fulfill diagnostic criteria. These restrictions often lead to diagnostic delays, potential misclassification of actual injury status, and provide little information regarding underlying cause. Novel biomarkers of damage have shown ability to reflect ongoing kidney injury and help further refine existing Risk, Injury, Failure, Loss, End-stage kidney disease (RIFLE) and Acute Kidney Injury Network (AKIN) diagnostic criteria. A comprehensive review of the published literature to date was performed using previously published methodology of the Acute Dialysis Quality Initiative (ADQI) working group to es-tablish consensus statements regarding (i) the overall implementation of injury biomarkers in the concept of AKI diagnosis, (ii) their clinical use, and (iii) future research. On the basis of published data on the ability of novel damage biomarkers to provide diagnostic and prognostic information on AKI, we recommend that novel damage biomarkers may, in the appropriate clinical setting and context (situation consistent with AKI), be used to diagnose AKI even in the absence of changes in serum creatinine or the presence of oliguria as described in the existing RIFLE/AKIN criteria for diagnosis of AKI. Adding injury biomarkers as a criterion for AKI will complement the ability of RIFLE/AKIN to define AKI. Promising diagnostic injury markers include neutrophil gelatinase-associated lipocalin (NGAL), kidney injury molecule 1 (KIM-1), interleukin 18 (IL-18) and liver-type fatty acid binding protein (L-FABP). However, there are currently insufficient data on damage biomarkers to support their use for AKI staging. Rigorous validation studies measuring the association between the novel damage biomarker(s) and clinically relevant outcomes are needed.
机译:急性肾脏损伤(AKI)通常发生在住院患者的患者中,并独立,并强烈地涉及发病率和死亡率。由于使用血清肌酸酐和尿醛征收来履行诊断标准,因此尚未完全实现及时和最明确的AKI诊断的临床益处。这些限制往往导致诊断延误,潜在的实际伤害状况的错误分类,并提供有关潜在原因的信息。损害的新型生物标志物已经表明了反映持续肾损伤的能力,并有助于进一步细化现有的风险,损伤,失败,丧失,终级肾病(步枪)和急性肾损伤网络(Akin)诊断标准。通过先前公布的急性透析质量倡议(ADQI)工作组的方法进行了全面审查发表的文献迄今为止的急性透析质量倡议(ADQI)工作组关于(i)关于(i)疾病诊断概念的伤害生物标志物的总体实施( ii)他们的临床使用,和(iii)未来的研究。在公布数据的基础上,关于新型损害生物标志物提供关于AKI的诊断和预后信息的基础,我们建议在适当的临床环境和背景下(与AKI一致的情况)的新型损伤生物标志物可以用于诊断AKI甚至在没有血清肌酐的变化或寡尿的存在,如现有步枪/ akin标准用于诊断AKI的标准。将伤害生物标志物添加为AKI的标准将补充步枪/类似地定义AKI的能力。有前途的诊断损伤标记包括中性粒细胞明胶酶相关的脂素(NGAL),肾损伤分子1(Kim-1),白细胞介素18(IL-18)和肝型脂肪酸结合蛋白(L-FABP)。然而,目前有足够的数据有关损坏生物标志物的数据,以支持他们对AKI分期的用途。需要严格的验证研究,测量新型损伤生物标志物之间的关联和临床相关结果。

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