确定重度恶性疟原虫疟疾非洲儿童严重代谢性酸中毒和尿毒症的预后因素：一项随机试验的二次分析。

Identifying prognostic factors of severe metabolic acidosis and uraemia in African children with severe falciparum malaria: a secondary analysis of a randomized trial.

机构信息

Malawi Liverpool Wellcome Trust, Queen Elizabeth Central Hospital College of Medicine, Chichiri 3, P.O. Box 30096, Blantyre, Malawi.

University of Malawi, College of Medicine, Blantyre, Malawi.

出版信息

Malar J. 2021 Jun 25;20(1):282. doi: 10.1186/s12936-021-03785-0.

DOI:10.1186/s12936-021-03785-0

PMID:34172046

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8234663/

Abstract

BACKGROUND

Severe metabolic acidosis and acute kidney injury are major causes of mortality in children with severe malaria but are often underdiagnosed in low resource settings.

METHODS

A retrospective analysis of the 'Artesunate versus quinine in the treatment of severe falciparum malaria in African children' (AQUAMAT) trial was conducted to identify clinical features of severe metabolic acidosis and uraemia in 5425 children from nine African countries. Separate models were fitted for uraemia and severe metabolic acidosis. Separate univariable and multivariable logistic regression were performed to identify prognostic factors for severe metabolic acidosis and uraemia. Both analyses adjusted for the trial arm. A forward selection approach was used for model building of the logistic models and a threshold of 5% statistical significance was used for inclusion of variables into the final logistic model. Model performance was assessed through calibration, discrimination, and internal validation with bootstrapping.

RESULTS

There were 2296 children identified with severe metabolic acidosis and 1110 with uraemia. Prognostic features of severe metabolic acidosis among them were deep breathing (OR: 3.94, CI 2.51-6.2), hypoglycaemia (OR: 5.16, CI 2.74-9.75), coma (OR: 1.72 CI 1.17-2.51), respiratory distress (OR: 1.46, CI 1.02-2.1) and prostration (OR: 1.88 CI 1.35-2.59). Features associated with uraemia were coma (3.18, CI 2.36-4.27), Prostration (OR: 1.78 CI 1.37-2.30), decompensated shock (OR: 1.89, CI 1.31-2.74), black water fever (CI 1.58. CI 1.09-2.27), jaundice (OR: 3.46 CI 2.21-5.43), severe anaemia (OR: 1.77, CI 1.36-2.29) and hypoglycaemia (OR: 2.77, CI 2.22-3.46) CONCLUSION: Clinical and laboratory parameters representing contributors and consequences of severe metabolic acidosis and uraemia were independently associated with these outcomes. The model can be useful for identifying patients at high risk of these complications where laboratory assessments are not routinely available.

摘要

背景

严重代谢性酸中毒和急性肾损伤是导致重症疟疾儿童死亡的主要原因，但在资源匮乏的环境中往往诊断不足。

方法

对“青蒿琥酯与奎宁治疗非洲儿童重症恶性疟”（AQUAMAT）试验进行回顾性分析，以确定来自 9 个非洲国家的 5425 名儿童中严重代谢性酸中毒和尿毒症的临床特征。分别为尿毒症和严重代谢性酸中毒建立单独的模型。分别进行单变量和多变量逻辑回归，以确定严重代谢性酸中毒和尿毒症的预后因素。两种分析均针对试验臂进行调整。使用向前选择方法构建逻辑模型，将统计学意义 5%的变量纳入最终逻辑模型。使用自举法评估逻辑模型的校准、区分和内部验证。

结果

共发现 2296 例严重代谢性酸中毒患儿和 1110 例尿毒症患儿。其中严重代谢性酸中毒的预后特征为深吸气（OR：3.94，CI 2.51-6.2）、低血糖（OR：5.16，CI 2.74-9.75）、昏迷（OR：1.72，CI 1.17-2.51）、呼吸困难（OR：1.46，CI 1.02-2.1）和乏力（OR：1.88，CI 1.35-2.59）。与尿毒症相关的特征包括昏迷（3.18，CI 2.36-4.27）、乏力（OR：1.78，CI 1.37-2.30）、失代偿性休克（OR：1.89，CI 1.31-2.74）、黑尿热（CI 1.58，CI 1.09-2.27）、黄疸（OR：3.46，CI 2.21-5.43）、严重贫血（OR：1.77，CI 1.36-2.29）和低血糖（OR：2.77，CI 2.22-3.46）。