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Comparison of blood smear, antigen detection, and nested-PCR methods for screening refugees from regions where malaria is endemic after a malaria outbreak in Quebec, Canada

机译:比较加拿大魁北克省疟疾暴发后疟疾流行地区的血液涂片,抗原检测和巢式PCR方法筛查难民

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摘要

The importation of malaria into a region where it is not endemic raises many concerns, including the timely delivery of appropriate care, safety of the blood supply, and the risk of autochthonous transmission. There is presently no consensus on the best way to screen mobile populations for malaria. Between August 2000 and March 2001, 535 refugees arrived in Quebec, Canada, from Tanzanian camps. Within 4 weeks of resettlement of the first group of 224, the McGill University Centre for Tropical Diseases noted an outbreak of malaria across the province (15 cases over a 3-week period). This group (group 1) was traced and screened for malaria between 3 and 4 months after arrival in Canada. Subsequent groups of 106 and 205 refugees were screened immediately upon arrival in Canada (group 2) and immediately prior to their departure from refugee camps (group 3), respectively. A single EDTA-blood sample was obtained from 521 refugees for testing by thick and thin blood smears (groups 1 and 2), antigen detection (ICT Malaria Pf and OptiMAL; group 1 only), and nested PCR (all groups). Overall, 98 of 521 refugees were found to be infected (18.8%). The vast majority of infections (81 of 98) were caused by Plasmodium falciparum alone. Using PCR as the "gold standard," both microscopy (sensitivity, 50%; specificity, 100%) and antigen detection (ICT sensitivity, 37.5%; ICT specificity, 100%; OptiMAL sensitivity, 29.1%; OptiMAL specificity, 95.6%) performed poorly. None of the PCR-positive subjects were symptomatic at the time of testing, and only two had recently had symptoms compatible with malaria (with or without diagnosis and treatment). Active surveillance of migrants from regions of intense malaria transmission can reduce the risk of morbidity in the migrant population and mitigate against transmission to the host population. Our data demonstrate that PCR is, by far, the most ++
机译:将疟疾输入到一个非地方性流行地区引起了很多关注,包括及时提供适当的护理,血液供应的安全性以及自发传播的风险。目前尚无关于筛查疟疾流动人口的最佳方法的共识。在2000年8月至2001年3月之间,有535名难民从坦桑尼亚难民营抵达加拿大魁北克。在第一批224人重新安置的4周内,麦吉尔大学热带病中心注意到全省爆发了疟疾(3周内有15例)。追踪该组(第1组)并在抵达加拿大后3-4个月进行疟疾筛查。随后分别有106和205难民群体在抵达加拿大(第2组)和离开难民营之前(第3组)进行了筛查。从521名难民中获得了一个EDTA血液样本,进行了浓血和稀血涂片检查(第1和2组),抗原检测(ICT疟疾Pf和OptiMAL;仅第1组)和巢式PCR(所有组)进行测试。总体而言,在521名难民中,有98名被感染(18.8%)。绝大多数感染(98个感染中的81个)仅由恶性疟原虫引起。使用PCR作为“金标准”,显微镜(灵敏度为50%;特异性为100%)和抗原检测(ICT灵敏度为37.5%; ICT特异性为100%;最优灵敏度为29.1%;最优特异性为95.6%)表现不佳。在测试时,没有一个PCR阳性受试者是有症状的,只有两个最近出现了与疟疾相适应的症状(有或没有诊断和治疗)。对来自疟疾传播严重地区的移民进行积极监测,可以减少移民人口患病的风险,并减轻其向宿主人口的传播。我们的数据表明,到目前为止,PCR是最++

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