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首页> 外文期刊>Malaria Journal >Estimation of heterogeneity in malaria transmission by stochastic modelling of apparent deviations from mass action kinetics
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Estimation of heterogeneity in malaria transmission by stochastic modelling of apparent deviations from mass action kinetics

机译:通过与质量作用动力学的明显偏差的随机建模估算疟疾传播中的异质性

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Background Quantifying heterogeneity in malaria transmission is a prerequisite for accurate predictive mathematical models, but the variance in field measurements of exposure overestimates true micro-heterogeneity because it is inflated to an uncertain extent by sampling variation. Descriptions of field data also suggest that the rate of Plasmodium falciparum infection is not proportional to the intensity of challenge by infectious vectors. This appears to violate the principle of mass action that is implied by malaria biology. Micro-heterogeneity may be the reason for this anomaly. It is proposed that the level of micro-heterogeneity can be estimated from statistical models that estimate the amount of variation in transmission most compatible with a mass-action model for the relationship of infection to exposure. Methods The relationship between the entomological inoculation rate (EIR) for falciparum malaria and infection risk was reanalysed using published data for cohorts of children in Saradidi (western Kenya). Infection risk was treated as binomially distributed, and measurement-error (Poisson and negative binomial) models were considered for the EIR. Models were fitted using Bayesian Markov chain Monte Carlo algorithms and model fit compared for models that assume either mass-action kinetics, facilitation, competition or saturation of the infection process with increasing EIR. Results The proportion of inocula that resulted in infection in Saradidi was inversely related to the measured intensity of challenge. Models of facilitation showed, therefore, a poor fit to the data. When sampling error in the EIR was neglected, either competition or saturation needed to be incorporated in the model in order to give a good fit. Negative binomial models for the error in exposure could achieve a comparable fit while incorporating the more parsimonious and biologically plausible mass action assumption. Models that assume negative binomial micro-heterogeneity predict lower incidence of infection at a given average exposure than do those assuming exposure to be uniform. The negative binomial model moreover provides an estimate of the variance of the within-cohort distribution of the EIR and hence of within cohort heterogeneity in exposure. Conclusion Apparent deviations from mass action kinetics in parasite transmission can arise from spatial and temporal heterogeneity in the inoculation rate, and from imprecision in its measurement. For parasites like P. falciparum, where there is no plausible biological rationale for deviations from mass action, this provides a strategy for estimating true levels of heterogeneity, since if mass-action is assumed, the within-population variance in exposure becomes identifiable in cohort studies relating infection to transmission intensity. Statistical analyses relating infection to exposure thus provide a valid general approach for estimating heterogeneity in transmission but only when they incorporate mass action kinetics and shrinkage estimates of exposure. Such analyses make it possible to include realistic levels of heterogeneity in dynamic models that predict the impact of control measures on transmission intensity.
机译:背景量化疟疾传播中的异质性是准确预测数学模型的先决条件,但是暴露现场测量中的差异过高估计了真实的微观异质性,因为通过采样变化将其异化膨胀到不确定的程度。现场数据说明还表明,恶性疟原虫的感染率与传染性载体的攻击强度不成比例。这似乎违反了疟疾生物学暗示的大规模行动原则。微观异质性可能是造成这种异常的原因。建议从统计模型估计微观异质性水平,该统计模型估计与感染与暴露之间的关系的质量作用模型最相容的传播变化量。方法使用公布的萨拉丁迪(肯尼亚西部)儿童队列数据重新分析恶性疟疾的昆虫接种率(EIR)与感染风险之间的关系。将感染风险视为二项分布,并针对EIR考虑测量误差(泊松和负二项式)模型。使用贝叶斯马尔可夫链蒙特卡洛算法对模型进行拟合,并对假设质量效应动力学,促进作用,竞争或感染过程随着EIR增加而饱和的模型进行模型拟合比较。结果在撒拉迪地区引起感染的接种比例与所测得的攻击强度呈反比关系。因此,便利化模型显示与数据的拟合度很差。当忽略EIR中的采样误差时,需要在模型中加入竞争或饱和度,以达到良好的拟合度。暴露误差的负二项式模型可以实现可比的拟合,同时结合更简约和生物学上合理的质量作用假设。假定负二项式微观异质性的模型预测的给定平均暴露水平下的感染率要低于假定均匀暴露的模型。此外,负二项式模型提供了对EIR人群内部分布的方差的估计,因此可以估算出暴露人群中人群内部异质性。结论寄生虫传播中与质量作用动力学的明显偏差可能是由于接种率的时空异质性以及其测量的不精确性引起的。对于恶性疟原虫(P.falciparum)等寄生虫,没有合理的生物学依据来解释偏离群聚作用的情况,这提供了一种估算真实异质性水平的策略,因为如果假设了群聚作用,则可以在队列研究中识别出人群内部的暴露差异。有关感染与传播强度的研究。因此,将感染与暴露相关的统计分析提供了一种有效的通用方法,可用于评估传播的异质性,但前提是它们必须结合质量作用动力学和暴露的收缩估计。这样的分析使得可以在预测控制措施对传输强度影响的动态模型中包括实际的异质性水平。

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