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无症状疟原虫感染清除率与克隆数量相互作用,可预测肯尼亚儿童后续疟疾的发病风险。

Clearance of asymptomatic P. falciparum Infections Interacts with the number of clones to predict the risk of subsequent malaria in Kenyan children.

机构信息

Infectious Diseases Unit, Department of Medicine Solna, Karolinska Institutet, Stockholm, Sweden.

出版信息

PLoS One. 2011 Feb 24;6(2):e16940. doi: 10.1371/journal.pone.0016940.

Abstract

BACKGROUND

Protective immunity to malaria is acquired after repeated infections in endemic areas. Asymptomatic multiclonal P. falciparum infections are common and may predict host protection. Here, we have investigated the effect of clearing asymptomatic infections on the risk of clinical malaria.

METHODS

Malaria episodes were continuously monitored in 405 children (1-6 years) in an area of moderate transmission, coastal Kenya. Blood samples collected on four occasions were assessed by genotyping the polymorphic P. falciparum merozoite surface protein 2 using fluorescent PCR and capillary electrophoresis. Following the second survey, asymptomatic infections were cleared with a full course of dihydroartemisinin.

RESULTS

Children who were parasite negative by PCR had a lower risk of subsequent malaria regardless of whether treatment had been given. Children with ≥ 2 clones had a reduced risk of febrile malaria compared with 1 clone after clearance of asymptomatic infections, but not if asymptomatic infections were not cleared. Multiclonal infection was associated with an increased risk of re-infection after drug treatment. However, among the children who were re-infected, multiclonal infections were associated with a shift from clinical malaria to asymptomatic parasitaemia.

CONCLUSION

The number of clones was associated with exposure as well as blood stage immunity. These effects were distinguished by clearing asymptomatic infection with anti-malarials. Exposure to multiple P. falciparum infections is associated with protective immunity, but there appears to be an additional effect in untreated multiclonal infections that offsets this protective effect.

摘要

背景

在流行地区反复感染后,可获得对疟疾的保护性免疫。无症状多克隆疟原虫感染很常见,可能预测宿主保护。在这里,我们研究了清除无症状感染对临床疟疾风险的影响。

方法

在肯尼亚沿海地区一个中度传播地区,连续监测了 405 名(1-6 岁)儿童的疟疾发作情况。通过荧光 PCR 和毛细管电泳对多态性疟原虫裂殖体表面蛋白 2 进行基因分型,对四次采集的血样进行评估。在第二次调查后,用全疗程双氢青蒿素清除无症状感染。

结果

无论是否进行治疗,PCR 检测为阴性的儿童随后发生疟疾的风险较低。与清除无症状感染前的 1 个克隆相比,清除无症状感染后的儿童中,≥ 2 个克隆的儿童发生发热性疟疾的风险降低,但如果不清除无症状感染则不会降低。多克隆感染与药物治疗后再感染的风险增加有关。然而,在接受再感染的儿童中,多克隆感染与从临床疟疾转为无症状寄生虫血症有关。

结论

克隆数量与暴露以及血液阶段免疫有关。这些影响通过用抗疟药物清除无症状感染来区分。接触多种疟原虫感染与保护性免疫有关,但在未经治疗的多克隆感染中似乎存在额外的影响,抵消了这种保护作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/15e8/3044709/f13e0192b12a/pone.0016940.g001.jpg

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