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Low Prevalence of Antibodies to Preerythrocytic but Not Blood-Stage Plasmodium falciparum Antigens in an Area of Unstable Malaria Transmission Compared to Prevalence in an Area of Stable Malaria Transmission▿

机译:与不稳定疟疾传播地区的患病率相比,不稳定疟疾传播地区中的红细胞前抗体但不是血站性恶性疟原虫抗原的患病率低▿

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摘要

In areas where levels of transmission of Plasmodium falciparum are high and stable, the age-related acquisition of high-level immunoglobulin G (IgG) antibodies to preerythrocytic circumsporozoite protein (CSP) and liver-stage antigen 1 (LSA-1) has been associated with protection from clinical malaria. In contrast, age-related protection from malaria develops slowly or not at all in residents of epidemic-prone areas with unstable low levels of malaria transmission. We hypothesized that this suboptimal clinical and parasitological immunity may in part be due to reduced antibodies to CSP or LSA-1 and/or vaccine candidate blood-stage antigens. Frequencies and levels of IgG antibodies to CSP, LSA-1, thrombospondin-related adhesive protein (TRAP), apical membrane antigen 1 (AMA-1), erythrocyte binding antigen 175 (EBA-175), and merozoite surface protein 1 (MSP-1) were compared in 243 Kenyans living in a highland area of unstable transmission and 210 residents of a nearby lowland area of stable transmission. Levels of antibodies to CSP, LSA-1, TRAP, and AMA-1 in the oldest age group (>40 years) in the unstable transmission area were lower than or similar to those of children 2 to 6 years old in the stable transmission area. Only 3.3% of individuals in the unstable transmission area had high levels of IgG (>2 arbitrary units) to both CSP and LSA-1, compared to 43.3% of individuals in the stable transmission area. In contrast, antibody levels to and frequencies of MSP-1 and EBA-175 were similar in adults in areas of stable and unstable malaria transmission. Suboptimal immunity to malaria in areas of unstable malaria transmission may relate in part to infrequent high-level antibodies to preerythrocytic antigens and AMA-1.
机译:在恶性疟原虫的传播水平高且稳定的地区,与年龄相关的抗红细胞前环子孢子蛋白(CSP)和肝阶段抗原1(LSA-1)的高水平免疫球蛋白G(IgG)抗体的获得有关可以预防临床疟疾。相比之下,与年龄有关的疟疾防护在疟疾传播水平不稳定的易流行地区的居民中发展缓慢或根本没有发展。我们假设这种次优的临床和寄生虫学免疫可能部分是由于针对CSP或LSA-1的抗体和/或疫苗候选血期抗原的抗体减少。抗CSP,LSA-1,血小板反应蛋白相关粘附蛋白(TRAP),顶膜抗原1(AMA-1),红细胞结合抗原175(EBA-175)和裂殖子表面蛋白1(MSP- 1)在生活在不稳定的高地地区的243名肯尼亚人和附近稳定传播的低地地区的210名居民进行了比较。不稳定传播区年龄最大(> 40岁)的CSP,LSA-1,TRAP和AMA-1抗体水平低于或接近稳定传播区2至6岁儿童的抗体水平。在不稳定的传播地区,只有3.3%的人对CSP和LSA-1的IgG含量较高(> 2个任意单位),而在稳定的传播地区,这一比例为43.3%。相反,在稳定和不稳定疟疾传播地区的成年人中,针对MSP-1和EBA-175的抗体水平和频率相似。在不稳定的疟疾传播地区,对疟疾的免疫力欠佳,可能部分与针对促红细胞生成前抗原和AMA-1的罕见高水平抗体有关。

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