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Predicting mortality for paediatric inpatients where malaria is uncommon

机译:预测疟疾不常见的小儿住院患者的死亡率

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Objective: As the proportion of children living low malaria transmission areas in sub-Saharan Africa increases, approaches for identifying non-malarial severe illness need to be evaluated to improve child outcomes. Design: As a prospective cohort study, we identified febrile paediatric inpatients, recorded data using Integrated Management of Childhood Illness (IMCI) criteria, and collected diagnostic specimens. Setting: Tertiary referral centre, northern Tanzania. Results: Of 466 participants with known outcome, median age was 1.4 years (range 2 months-13.0 years), 200 (42.9%) were female, 11 (2.4%) had malaria and 34 (7.3%) died. Inpatient death was associated with: Capillary refill >3 s (OR 9.0, 95% CI 3.0 to 26.7), inability to breastfeed or drink (OR 8.9, 95% CI 4.0 to 19.6), stiff neck (OR 7.0, 95% CI 2.8 to 17.6), lethargy (OR 5.2, 95% CI 2.5 to 10.6), skin pinch >2 s (OR 4.8, 95% CI 1.9 to 12.3), respiratory difficulty (OR 4.0, 95% CI 1.9 to 8.2), generalised lymphadenopathy (OR 3.6, 95% CI 1.6 to 8.3) and oral candidiasis (OR 3.4, 95% CI 1.4 to 8.3). BCS <5 (OR 27.2, p<0.001) and severe wasting (OR 6.9, p<0.001) were independently associated with inpatient death. Conclusions: In a low malaria transmission setting, IMCI criteria performed well for predicting inpatient death from non-malarial illness. Laboratory results were not as useful in predicting death, underscoring the importance of clinical examination in assessing prognosis. Healthcare workers should consider local malaria epidemiology as malaria over-diagnosis in children may delay potentially life-saving interventions in areas where malaria is uncommon.
机译:目的:随着撒哈拉以南非洲低疟疾传播地区儿童的比例增加,需要评估确定非疟疾严重疾病的方法,以改善儿童的结局。设计:作为一项前瞻性队列研究,我们确定了高热儿科住院患者,使用儿童疾病综合管理(IMCI)标准记录了数据,并收集了诊断标本。地点:坦桑尼亚北部的第三级转诊中心。结果:在466名已知结局的参与者中,中位年龄为1.4岁(范围为2个月至13.0岁),其中200名女性(42.9%)为女性,11名女性(2.4%)患有疟疾,34名(7.3%)死亡。住院死亡与以下原因有关:毛细血管补充> 3 s(OR 9.0,95%CI 3.0至26.7),无法母乳喂养或饮水(OR 8.9,95%CI 4.0至19.6),脖子僵硬(OR 7.0,95%CI 2.8至17.6),嗜睡(OR 5.2、95%CI 2.5至10.6),皮肤捏痛> 2 s(OR 4.8、95%CI 1.9至12.3),呼吸困难(OR 4.0、95%CI 1.9至8.2),广泛性淋巴结病(OR 3.6,95%CI 1.6至8.3)和口腔念珠菌病(OR 3.4,95%CI 1.4至8.3)。 BCS <5(OR 27.2,p <0.001)和严重消瘦(OR 6.9,p <0.001)与住院死亡独立相关。结论:在低疟疾传播环境中,IMCI标准在预测非疟疾住院死亡方面表现良好。实验室检查结果对预测死亡没有帮助,强调了临床检查对评估预后的重要性。医护人员应考虑当地的疟疾流行病学,因为对儿童的疟疾过度诊断可能会延迟在疟疾罕见的地区可能挽救生命的干预措施。

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