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开发一种针对严重疟疾贫血的新型风险预测模型。

Developing a novel risk prediction model for severe malarial anemia.

作者信息

Brickley E B, Kabyemela E, Kurtis J D, Fried M, Wood A M, Duffy P E

机构信息

Laboratory of Malaria Immunology and Vaccinology, Division of Intramural Research, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rockville, Maryland, USA.

Department of Public Health and Primary Care, University of Cambridge, Cambridge, UK.

出版信息

Glob Health Epidemiol Genom. 2017 Sep 11;2:e14. doi: 10.1017/gheg.2017.8. eCollection 2017.

Abstract

As a pilot study to investigate whether personalized medicine approaches could have value for the reduction of malaria-related mortality in young children, we evaluated questionnaire and biomarker data collected from the Mother Offspring Malaria Study Project birth cohort (Muheza, Tanzania, 2002-2006) at the time of delivery as potential prognostic markers for pediatric severe malarial anemia. Severe malarial anemia, defined here as a infection accompanied by hemoglobin levels below 50 g/L, is a key manifestation of life-threatening malaria in high transmission regions. For this study sample, a prediction model incorporating cord blood levels of interleukin-1β provided the strongest discrimination of severe malarial anemia risk with a C-index of 0.77 (95% CI 0.70-0.84), whereas a pragmatic model based on sex, gravidity, transmission season at delivery, and bed net possession yielded a more modest C-index of 0.63 (95% CI 0.54-0.71). Although additional studies, ideally incorporating larger sample sizes and higher event per predictor ratios, are needed to externally validate these prediction models, the findings provide proof of concept that risk score-based screening programs could be developed to avert severe malaria cases in early childhood.

摘要

作为一项探索个性化医疗方法对于降低幼儿疟疾相关死亡率是否具有价值的试点研究,我们评估了从母婴疟疾研究项目出生队列(坦桑尼亚穆赫扎,2002 - 2006年)分娩时收集的问卷和生物标志物数据,将其作为小儿严重疟疾贫血的潜在预后标志物。严重疟疾贫血在此定义为伴有血红蛋白水平低于50 g/L的感染,是高传播地区危及生命的疟疾的关键表现。对于本研究样本,一个纳入脐带血白细胞介素-1β水平的预测模型对严重疟疾贫血风险的区分能力最强,C指数为0.77(95%置信区间0.70 - 0.84),而基于性别、妊娠次数、分娩时的传播季节和蚊帐拥有情况的实用模型C指数则较为适中,为0.63(95%置信区间0.54 - 0.71)。尽管需要开展更多研究(理想情况下纳入更大样本量和更高的预测指标事件比)来对这些预测模型进行外部验证,但这些发现提供了概念验证,即可以开发基于风险评分的筛查项目以避免幼儿期的严重疟疾病例。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/889d/5870436/019475583d14/S2054420017000082_fig1.jpg

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