首页> 美国卫生研究院文献>PLoS Neglected Tropical Diseases >The Incidence and Differential Seasonal Patterns of Plasmodium vivax Primary Infections and Relapses in a Cohort of Children in Papua New Guinea
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The Incidence and Differential Seasonal Patterns of Plasmodium vivax Primary Infections and Relapses in a Cohort of Children in Papua New Guinea

机译:巴布亚新几内亚一群儿童间日疟原虫感染和复发的发病率和季节性差异

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摘要

Plasmodium vivax has the ability to relapse from dormant parasites in the liver weeks or months after inoculation, causing further blood-stage infection and potential onward transmission. Estimates of the force of blood-stage infections arising from primary infections and relapses are important for designing intervention strategies. However, in endemic settings their relative contributions are unclear. Infections are frequently asymptomatic, many individuals harbor multiple infections, and while high-resolution genotyping of blood samples enables individual infections to be distinguished, primary infections and relapses cannot be identified. We develop a model and fit it to longitudinal genotyping data from children in Papua New Guinea to estimate the incidence and seasonality of P vivax primary infection and relapse. The children, aged one to three years at enrolment, were followed up over 16 months with routine surveys every two months. Blood samples were taken at the routine visits and at other times if the child was ill. Samples positive by microscopy or a molecular method for species detection were genotyped using high-resolution capillary electrophoresis for P vivax MS16 and msp1F3, and P falciparum msp2. The data were summarized as longitudinal patterns of success or failure to detect a genotype at each routine time-point (eg 001000001). We assume that the seasonality of P vivax primary infection is similar to that of P falciparum since they are transmitted by the same vectors and, because P falciparum does not have the ability to relapse, the seasonality can be estimated. Relapses occurring during the study period can be a consequence of infections occurring prior to the study: we assume that the seasonal pattern of primary infections repeats over time. We incorporate information from parasitological and entomology studies to gain leverage for estimating the parameters, and take imperfect detection into account. We estimate the force of P vivax primary infections to be 11.5 (10.5, 12.3) for a three-year old child per year and the mean number of relapses per infection to be 4.3 (4.0, 4.6) over 16 months. The peak incidence of relapses occurred in the two month interval following the peak interval for primary infections: the contribution to the force of blood-stage infection from relapses is between 71% and 90% depending on the season. Our estimates contribute to knowledge of the P vivax epidemiology and have implications for the timing of intervention strategies targeting different stages of the life cycle.
机译:间日疟原虫具有从接种后数周或数月的肝脏中休眠的寄生虫中复发的能力,从而导致进一步的血液感染和潜在的继续传播。由原发性感染和复发引起的血液阶段感染力的估算对于设计干预策略很重要。但是,在地方性环境中,它们的相对作用尚不清楚。感染通常是无症状的,许多人具有多种感染,并且对血液样本进行高分辨率基因分型可以区分个体感染,但无法确定原发性感染和复发。我们开发了一个模型并将其与来自巴布亚新几内亚儿童的纵向基因分型数据相符,以估计间日疟原虫感染和复发的发生率和季节性。在入学时年龄为1至3岁的儿童,每16个月进行一次随访,每两个月进行例行检查。在例行检查时以及在孩子生病时的其他时间采集血样。使用高分辨率毛细管电泳对间日疟原虫MS16和msp1F3以及恶性疟原虫msp2进行显微镜检查或分子检测阳性的样本进行基因分型。数据汇总为在每个常规时间点(例如001000001)检测基因型成功或失败的纵向模式。我们假设间日疟原虫感染的季节性与恶性疟原虫相似,因为它们是通过相同的载体传播的,并且由于恶性疟原虫不具有复发能力,因此可以估计其季节性。在研究期间发生的复发可能是在研究之前发生感染的结果:我们假设原发感染的季节性模式会随着时间重复。我们结合了寄生虫学和昆虫学研究的信息,以获取估计参数的能力,并考虑了不完善的检测。我们估计,对于一个三岁的孩子,每年间间日疟原虫感染的力量为11.5(10.5,12.3),在16个月内,每次感染的平均复发次数为4.3(4.0,4.6)。复发的峰值发生在原发感染高峰间隔后的两个月间隔内:根据季节,复发对血液阶段感染力的贡献在71%至90%之间。我们的估计有助于了解间日疟流行病学,并对针对生命周期不同阶段的干预策略的时机产生影响。

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