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当基于肌酐的电子警报发生变化时,儿科急性肾损伤的发生率会增加。

The incidence of pediatric acute kidney injury is increased when identified by a change in a creatinine-based electronic alert.

机构信息

Welsh Renal Clinical Network, Cwm Taf University Health Board.

Department of Clinical Biochemistry, Hywel Dda University Health Board.

出版信息

Kidney Int. 2017 Aug;92(2):432-439. doi: 10.1016/j.kint.2017.03.009. Epub 2017 May 6.

Abstract

A prospective national cohort study was undertaken to collect data on all cases of pediatric (under 18 yrs of age) acute kidney injury (AKI) identified by a biochemistry-based electronic alert using the Welsh National electronic AKI reporting system. Herein we describe the utility and limitation of using this modification of the KDIGO creatinine-based system data set to characterize pediatric AKI. Of 1,343 incident episodes over a 30-month period, 34.5% occurred in neonates of which 83.8% were AKI stage 1. Neonatal 30-day mortality was 4.1%, with 73.3% of this being accounted for by patients treated in an Intensive Care Unit. In the non-neonatal group, 76.1% were AKI stage 1. Hospital-acquired AKI accounted for 40.1% of episodes while community-acquired AKI represented 29.4% of cases within which 33.9% were admitted to hospital and 30.5% of cases were unclassified. Non-neonatal 30-day mortality was 1.2%, with half of this accounted for by patients treated in the Intensive Care Unit. Nonrecovery of renal function at 30 days occurred in 28% and was significantly higher in patients not admitted to hospital (45% vs. 20%). The reported incidence of AKI in children was far greater than previously reported in studies reliant on clinical identification of adult AKI or hospital coding data. Mortality was highest in neonates and driven by those in the Intensive Care Unit. Nonrecovery of renal function and persistent renal impairment was more common in non-neonates and was especially high in patients with community-acquired AKI who were not hospitalized.

摘要

一项前瞻性全国队列研究旨在通过使用威尔士国家电子急性肾损伤报告系统的基于生化的电子警报,收集所有儿科(18 岁以下)急性肾损伤(AKI)病例的数据。在此,我们描述了使用这种基于 KDIGO 肌酐系统数据集的修改版来描述儿科 AKI 的效用和局限性。在 30 个月的时间里,共发生了 1343 例新发病例,其中 34.5%发生在新生儿中,其中 83.8%为 AKI 1 期。新生儿 30 天死亡率为 4.1%,其中 73.3%归因于在重症监护病房接受治疗的患者。在非新生儿组中,76.1%为 AKI 1 期。医院获得性 AKI 占 40.1%,社区获得性 AKI 占 29.4%,其中 33.9%住院,30.5%未分类。非新生儿 30 天死亡率为 1.2%,其中一半归因于在重症监护病房接受治疗的患者。30 天时肾功能未恢复的发生率为 28%,在未住院的患者中明显更高(45%比 20%)。报告的儿童 AKI 发生率远远高于以前依赖成人 AKI 的临床识别或医院编码数据的研究。死亡率在新生儿中最高,主要由重症监护病房中的患者驱动。肾功能未恢复和持续肾损害在非新生儿中更为常见,在未住院的社区获得性 AKI 患者中尤其如此。

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