Mårtensson Johan, Jonsson Niklas, Glassford Neil J, Bell Max, Martling Claes-Roland, Bellomo Rinaldo, Larsson Anders
Section of Anaesthesia and Intensive Care Medicine, Department of Physiology and Pharmacology, Karolinska Institutet, Solnavägen 1, 171 77, Solna, Sweden.
Department of Intensive Care, Austin Hospital, 145 Studley Road, Heidelberg, VIC, 3084, Australia.
Ann Intensive Care. 2016 Dec;6(1):6. doi: 10.1186/s13613-016-0108-x. Epub 2016 Jan 13.
Breakdown of renal endothelial, tubular and glomerular matrix collagen plays a major role in acute kidney injury (AKI) development. Such collagen breakdown releases endostatin into the circulation. The aim of this study was to compare the AKI predictive value of plasma endostatin with two previously suggested biomarkers of AKI, cystatin C and neutrophil gelatinase-associated lipocalin (NGAL).
We studied 93 patients without kidney disease who had a first plasma sample obtained within 48 h of ICU admission. We identified risk factors for AKI within the population and designed a predictive model. The individual ability and net contribution of endostatin, cystatin C and NGAL to predict AKI were evaluated by the area under the receiver operating characteristics curve (AUC), likelihood-ratio test, net reclassification improvement (NRI) and integrated discrimination improvement (IDI).
In total, 21 (23 %) patients experienced AKI within 72 h. A three-parameter model (age, illness severity score and early oliguria) predicted AKI with an AUC of 0.759 (95 % CI 0.646-0.872). Adding endostatin to the predictive model significantly (P = 0.04) improved the AUC to 0.839 (95 % CI 0.752-0.925). In addition, endostatin significantly improved risk prediction using the likelihood-ratio test (P = 0.005), NRI analysis (0.27; P = 0.04) and IDI analysis (0.07; P = 0.04). In contrast, adding cystatin C or NGAL to the three-parameter model did not improve risk prediction in any of the four analyses.
In this cohort of critically ill patients, plasma endostatin improved AKI prediction based on clinical risk factors, while cystatin C and NGAL did not.
肾内皮、肾小管和肾小球基质胶原蛋白的分解在急性肾损伤(AKI)的发展中起主要作用。这种胶原蛋白分解会将内皮抑素释放到循环中。本研究的目的是比较血浆内皮抑素与两种先前提出的AKI生物标志物——胱抑素C和中性粒细胞明胶酶相关脂质运载蛋白(NGAL)对AKI的预测价值。
我们研究了93例无肾脏疾病的患者,这些患者在入住重症监护病房(ICU)后48小时内采集了首次血浆样本。我们确定了该人群中AKI的危险因素并设计了一个预测模型。通过受试者操作特征曲线(AUC)下面积、似然比检验、净重新分类改善(NRI)和综合判别改善(IDI)来评估内皮抑素、胱抑素C和NGAL预测AKI的个体能力和净贡献。
共有21例(23%)患者在72小时内发生了AKI。一个三参数模型(年龄、疾病严重程度评分和早期少尿)预测AKI的AUC为0.759(95%CI 0.646 - 0.872)。将内皮抑素添加到预测模型中显著(P = 0.04)提高了AUC至0.839(95%CI 0.752 - 0.925)。此外,使用似然比检验(P = 0.005)、NRI分析(0.27;P = 0.04)和IDI分析(0.07;P = 0.04)时,内皮抑素显著改善了风险预测。相比之下,将胱抑素C或NGAL添加到三参数模型中,在四项分析中的任何一项中都没有改善风险预测。
在这组重症患者中,血浆内皮抑素基于临床危险因素改善了AKI预测,而胱抑素C和NGAL则没有。
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