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不同程度暴露于疟疾传播对学龄前儿童抗疟抗体反应发展的影响。第十六部分。阿森博湾队列项目。

The effects of varying exposure to malaria transmission on development of antimalarial antibody responses in preschool children. XVI. Asembo Bay Cohort Project.

作者信息

Singer Lauren M, Mirel Lisa B, ter Kuile Feiko O, Branch OraLee H, Vulule John M, Kolczak Margarette S, Hawley William A, Kariuki Simon K, Kaslow David C, Lanar David E, Lal Altaf A

机构信息

Division of Parasitic Diseases, National Center for Infectious Diseases, Centers for Disease Control and Prevention, Atlanta, Georgia 30341-3717, USA.

出版信息

J Infect Dis. 2003 Jun 1;187(11):1756-64. doi: 10.1086/375241. Epub 2003 May 12.

Abstract

In areas of intense malaria transmission, malaria morbidity and mortality is highest in children 3-18 months old. Interventions that reduce malaria exposure early in life reduce morbidity but may also delay development of clinical immunity. We assessed the relationship between intensity of malaria exposure and development of antibody responses. Thirty-nine children were monitored monthly, from birth to > or =2.5 years old (1238 observations), and were divided into 3 exposure categories, on the basis of parasitemic episodes or entomological data. Children with low exposure during the first 2 years of life had higher subsequent levels of antibody to merozoite surface protein-1(19-kDa) (a marker of blood-stage responses) by months 24-35 (P<.05). This inverse relationship decreased as children aged. There was no consistent relationship between exposure early in life and subsequent levels of antibody to circumsporozoite protein (a marker of sporozoite-stage responses). These data suggest that, in areas of intense malaria transmission, during the first 3 years of life, interventions that either reduce the number of asexual parasitemic episodes or lower entomological exposure do not delay the development of antibody responses to blood-stage malarial antigens.

摘要

在疟疾传播猖獗的地区,3至18个月大的儿童疟疾发病率和死亡率最高。在生命早期减少疟疾暴露的干预措施可降低发病率,但也可能延迟临床免疫力的发展。我们评估了疟疾暴露强度与抗体反应发展之间的关系。39名儿童从出生到2.5岁及以上每月接受监测(共1238次观察),并根据寄生虫血症发作情况或昆虫学数据分为3个暴露类别。在生命的头两年暴露程度较低的儿童,在24至35个月时,对裂殖子表面蛋白-1(19-kDa)(血液阶段反应的标志物)的抗体水平较高(P<0.05)。随着儿童年龄增长,这种反比关系减弱。生命早期的暴露与随后环子孢子蛋白抗体水平(子孢子阶段反应的标志物)之间没有一致的关系。这些数据表明,在疟疾传播猖獗的地区,在生命的头3年里,减少无性寄生虫血症发作次数或降低昆虫学暴露的干预措施不会延迟对血液阶段疟疾抗原的抗体反应的发展。

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