早期序贯风险分层评估以优化急性肾损伤危重儿童的液体剂量、CRRT起始和终止:聚焦2过程文章

Jean-Philippe Roy, K. Krallman, Rajit K. Basu, R. Chima, Lin Fei, Sarah Wilder, A. Schmerge, Bradley Gerhardt, Kaylee Fox, Cassie L. Kirby, S. Goldstein
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引用次数: 5

摘要

背景:急性肾损伤(AKI)在危重儿童中很常见,并与发病率和死亡率增加有关。AKI的识别和管理往往延迟,使患者易患临床上显著的液体积聚(液体过载(FO))。对高危患者的早期识别和干预可降低与液体相关的发病率。我们的目标是评估AKI临床决策算法(CDA),使用顺序风险分层策略整合肾性心绞痛指数(RAI),尿中性粒细胞明胶酶相关脂钙蛋白(NGAL)和速尿压力测试(FST),以优化AKI和FO的预测和管理危重儿童。方法/设计:本单中心前瞻性观察队列研究评估儿科重症监护病房(PICU)的AKI CDA。每个≥3个月的患者在入院12小时自动计算风险评分RAI。RAI≥8(满足肾性心绞痛)的患者通过尿液NGAL进一步分层,如果NGAL阳性(NGAL≥150ng/mL),随后通过他们对标准剂量呋赛米(即FST)的反应进行分层。RAI阴性或NGAL阴性患者按常规护理进行治疗。快速反应者接受保守治疗,无反应者接受液体限制性治疗和/或持续肾替代治疗(CRRT),治疗比例为10%-15%。2100名患者将在3年内进行评估,包括210名严重AKI患者(KDIGO期2或3期AKI), 100名bbb10 % FO患者和50名需要CRRT的患者。主要分析:标准化儿童FST,评估CDA对儿童严重AKI的预测准确性、FO - 10%和CRRT需求。AKI患者的二次分析:28天内肾功能恢复基线、RRT和死亡率。讨论:这将是AKI CDA可行性的第一个前瞻性评估,将个体预测工具整合在一个有凝聚力和全面的方法中,以及它对FO bbbb10 %和AKI的预测,以及第一个标准化儿科人群FST的研究。这将增加对当前AKI预测工具的了解,并为危重儿童基于其风险水平的早期干预提供可操作的见解。
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Early Sequential Risk Stratification Assessment to Optimize Fluid Dosing, CRRT Initiation and Discontinuation in Critically Ill Children with Acute Kidney Injury: Taking Focus 2 Process Article
Background: Acute Kidney Injury (AKI) is common in critically ill children and is associated with increased morbidity and mortality. Recognition and management of AKI is often delayed, predisposing patients to risk of clinically significant fluid accumulation (Fluid Overload (FO)). Early recognition and intervention in high risk patients could decrease fluid associated morbidity. We aim to assess an AKI Clinical Decision Algorithm (CDA) using a sequential risk stratification strategy integrating the Renal Angina Index (RAI), urine Neutrophil Gelatinase-Associated Lipocalin (NGAL) and the Furosemide Stress Test (FST) to optimize AKI and FO prediction and management in critically ill children. Methods/Design: This single center prospective observational cohort study evaluates the AKI CDA in a Pediatric Intensive Care Unit (PICU). Every patient ≥ 3 months old has the risk score RAI calculated automatically at 12 hours of admission. Patients with a RAI ≥ 8 (fulfilling renal angina) have risk further stratified with a urine NGAL and, if positive (NGAL ≥ 150ng/mL), subsequently by their response to a standardized dose of furosemide (namely FST). RAI negative or NGAL negative patients are treated per usual care. FST-responders are managed conservatively, while non-responders receive fluid restrictive strategy and/or continuous renal replacement therapy (CRRT) at 10%-15% of FO. 2100 patients over 3 years will be evaluated to capture 210 patients with severe AKI (KDIGO Stage 2 or 3 AKI), 100 patients with >10% FO, and 50 requiring CRRT. Primary analyses: Standardizing a pediatric FST and assessing prediction accuracy of CDA for severe AKI, FO>10% and CRRT requirement in children. Secondary analyses in patients with AKI: Renal function return to baseline, RRT and mortality within 28 days. Discussion: This will be the first prospective evaluation of feasibility of AKI CDA, integrating individual prediction tools in one cohesive and comprehensive approach, and its prediction of FO>10% and AKI, as well as the first to standardize the FST in the pediatric population. This will increase knowledge on current AKI prediction tools and provide actionable insight for early interventions in critically ill children based on their level of risk.
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