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一份关于为发展中国家麻疹动态模型设定参数所需数据的综述。

A review of data needed to parameterize a dynamic model of measles in developing countries.

作者信息

Szusz Emily K, Garrison Louis P, Bauch Chris T

机构信息

Department of Mathematics and Statistics, University of Guelph, Guelph, Canada.

出版信息

BMC Res Notes. 2010 Mar 16;3:75. doi: 10.1186/1756-0500-3-75.

Abstract

BACKGROUND

Dynamic models of infection transmission can project future disease burden within a population. Few dynamic measles models have been developed for low-income countries, where measles disease burden is highest. Our objective was to review the literature on measles epidemiology in low-income countries, with a particular focus on data that are needed to parameterize dynamic models.

METHODS

We included age-stratified case reporting and seroprevalence studies with fair to good sample sizes for mostly urban African and Indian populations. We emphasized studies conducted before widespread immunization. We summarized age-stratified attack rates and seroprevalence profiles across these populations. Using the study data, we fitted a "representative" seroprevalence profile for African and Indian settings. We also used a catalytic model to estimate the age-dependent force of infection for individual African and Indian studies where seroprevalence was surveyed. We used these data to quantify the effects of population density on the basic reproductive number R0.

RESULTS

The peak attack rate usually occurred at age 1 year in Africa, and 1 to 2 years in India, which is earlier than in developed countries before mass vaccination. Approximately 60% of children were seropositive for measles antibody by age 2 in Africa and India, according to the representative seroprevalence profiles. A statistically significant decline in the force of infection with age was found in 4 of 6 Indian seroprevalence studies, but not in 2 African studies. This implies that the classic threshold result describing the critical proportion immune (pc) required to eradicate an infectious disease, pc = 1-1/R0, may overestimate the required proportion immune to eradicate measles in some developing country populations. A possible, though not statistically significant, positive relation between population density and R0 for various Indian and African populations was also found. These populations also showed a similar pattern of waning of maternal antibodies. Attack rates in rural Indian populations show little dependence on vaccine coverage or population density compared to urban Indian populations. Estimated R0 values varied widely across populations which has further implications for measles elimination.

CONCLUSIONS

It is possible to develop a broadly informative dynamic model of measles transmission in low-income country settings based on existing literature, though it may be difficult to develop a model that is closely tailored to any given country. Greater efforts to collect data specific to low-income countries would aid in control efforts by allowing highly population-specific models to be developed.

摘要

背景

感染传播的动态模型可以预测人群未来的疾病负担。针对低收入国家(麻疹疾病负担最高的地区)开发的动态麻疹模型很少。我们的目标是回顾低收入国家麻疹流行病学的文献,特别关注参数化动态模型所需的数据。

方法

我们纳入了年龄分层的病例报告和血清阳性率研究,这些研究针对主要为非洲和印度城市人口的样本量适中至良好的情况。我们强调在广泛免疫之前进行的研究。我们总结了这些人群中年龄分层的发病率和血清阳性率概况。利用研究数据,我们拟合了非洲和印度地区的“代表性”血清阳性率概况。我们还使用催化模型来估计在进行血清阳性率调查的各个非洲和印度研究中年龄依赖性感染强度。我们利用这些数据来量化人口密度对基本再生数R0的影响。

结果

在非洲,发病率峰值通常出现在1岁,在印度出现在1至2岁,这比大规模疫苗接种前的发达国家更早。根据代表性血清阳性率概况,在非洲和印度,约60%的儿童在2岁时麻疹抗体呈血清阳性。在6项印度血清阳性率研究中的4项中发现感染强度随年龄有统计学显著下降,但在2项非洲研究中未发现。这意味着描述根除传染病所需的临界免疫比例(pc)的经典阈值结果,即pc = 1 - 1/R0,可能高估了一些发展中国家人群中根除麻疹所需的免疫比例。还发现不同印度和非洲人群的人口密度与R0之间可能存在正相关关系,尽管无统计学显著性。这些人群还表现出母体抗体衰减的相似模式。与印度城市人口相比,印度农村人口的发病率对疫苗接种覆盖率或人口密度的依赖性较小。估计的R0值在不同人群中差异很大,这对麻疹消除有进一步影响。

结论

根据现有文献,有可能在低收入国家背景下开发一个具有广泛信息的麻疹传播动态模型,尽管可能难以开发一个完全针对任何特定国家的模型。加大收集低收入国家特定数据的力度,将有助于通过开发高度针对特定人群的模型来进行控制工作。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/045a/2848058/e105d107f7ce/1756-0500-3-75-1.jpg

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