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13价肺炎球菌结合疫苗对马拉维中部儿童三年临床及低氧血症性肺炎的影响:一项观察性研究

Impact of the 13-Valent Pneumococcal Conjugate Vaccine on Clinical and Hypoxemic Childhood Pneumonia over Three Years in Central Malawi: An Observational Study.

作者信息

McCollum Eric D, Nambiar Bejoy, Deula Rashid, Zadutsa Beatiwel, Bondo Austin, King Carina, Beard James, Liyaya Harry, Mankhambo Limangeni, Lazzerini Marzia, Makwenda Charles, Masache Gibson, Bar-Zeev Naor, Kazembe Peter N, Mwansambo Charles, Lufesi Norman, Costello Anthony, Armstrong Ben, Colbourn Tim

机构信息

Institute for Global Health, University College London, London, United Kingdom.

Department of Pediatrics, Division of Pulmonology, Johns Hopkins School of Medicine, Baltimore, Maryland, United States of America.

出版信息

PLoS One. 2017 Jan 4;12(1):e0168209. doi: 10.1371/journal.pone.0168209. eCollection 2017.

Abstract

BACKGROUND

The pneumococcal conjugate vaccine's (PCV) impact on childhood pneumonia during programmatic conditions in Africa is poorly understood. Following PCV13 introduction in Malawi in November 2011, we evaluated the case burden and rates of childhood pneumonia.

METHODS AND FINDINGS

Between January 1, 2012-June 30, 2014 we conducted active pneumonia surveillance in children <5 years at seven hospitals, 18 health centres, and with 38 community health workers in two districts, central Malawi. Eligible children had clinical pneumonia per Malawi guidelines, defined as fast breathing only, chest indrawing +/- fast breathing, or, ≥1 clinical danger sign. Since pulse oximetry was not in the Malawi guidelines, oxygenation <90% defined hypoxemic pneumonia, a distinct category from clinical pneumonia. We quantified the pneumonia case burden and rates in two ways. We compared the period immediately following vaccine introduction (early) to the period with >75% three-dose PCV13 coverage (post). We also used multivariable time-series regression, adjusting for autocorrelation and exploring seasonal variation and alternative model specifications in sensitivity analyses. The early versus post analysis showed an increase in cases and rates of total, fast breathing, and indrawing pneumonia and a decrease in danger sign and hypoxemic pneumonia, and pneumonia mortality. At 76% three-dose PCV13 coverage, versus 0%, the time-series model showed a non-significant increase in total cases (+47%, 95% CI: -13%, +149%, p = 0.154); fast breathing cases increased 135% (+39%, +297%, p = 0.001), however, hypoxemia fell 47% (-5%, -70%, p = 0.031) and hospital deaths decreased 36% (-1%, -58%, p = 0.047) in children <5 years. We observed a shift towards disease without danger signs, as the proportion of cases with danger signs decreased by 65% (-46%, -77%, p<0.0001). These results were generally robust to plausible alternative model specifications.

CONCLUSIONS

Thirty months after PCV13 introduction in Malawi, the health system burden and rates of the severest forms of childhood pneumonia, including hypoxemia and death, have markedly decreased.

摘要

背景

肺炎球菌结合疫苗(PCV)在非洲计划免疫条件下对儿童肺炎的影响尚不清楚。2011年11月PCV13在马拉维引入后,我们评估了儿童肺炎的病例负担和发病率。

方法与结果

2012年1月1日至2014年6月30日期间,我们在马拉维中部两个地区的7家医院、18个健康中心以及38名社区卫生工作者中,对5岁以下儿童进行了肺炎主动监测。符合条件的儿童根据马拉维指南诊断为临床肺炎,定义为仅呼吸急促、胸凹陷伴/不伴呼吸急促或≥1个临床危险体征。由于脉搏血氧饱和度测定未纳入马拉维指南,氧合<90%定义为低氧血症性肺炎,这是与临床肺炎不同的类别。我们通过两种方式对肺炎病例负担和发病率进行了量化。我们比较了疫苗引入后立即的时期(早期)和三剂PCV13覆盖率>75%的时期(后期)。我们还使用了多变量时间序列回归,对自相关进行了调整,并在敏感性分析中探索了季节性变化和替代模型规格。早期与后期分析显示,总体、呼吸急促和胸凹陷性肺炎的病例数和发病率增加,危险体征和低氧血症性肺炎以及肺炎死亡率下降。在三剂PCV13覆盖率为76%时,与0%相比,时间序列模型显示总体病例数无显著增加(+47%,95%CI:-13%,+149%,p = 0.154);呼吸急促病例增加了135%(+39%,+297%,p = 0.001),然而,5岁以下儿童的低氧血症下降了47%(-5%,-70%,p = 0.031),医院死亡人数下降了36%(-1%,-58%,p = 0.047)。我们观察到向无危险体征疾病的转变,因为有危险体征的病例比例下降了65%(-46%,-77%,p<0.0001)。这些结果对于合理的替代模型规格通常是稳健的。

结论

在马拉维引入PCV13 30个月后,包括低氧血症和死亡在内的最严重形式的儿童肺炎的卫生系统负担和发病率显著下降。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0d6c/5215454/d20dd59d2056/pone.0168209.g001.jpg

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