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Antibodies to pre-erythrocytic Plasmodium falciparum antigens and risk of clinical malaria in Kenyan children

机译:肯尼亚儿童前红细胞恶性疟原虫抗原的抗体和临床疟疾的风险

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摘要

BACKGROUND: IgG antibodies to pre-erythrocytic antigens are involved in prevention of infection and disease in animal models of malaria but have not been associated with protection against disease in human malaria.METHODS: Levels of IgG antibodies to circumsporozoite protein (CSP), liver-stage antigen type 1 (LSA-1), and thrombospondin-related adhesive protein (TRAP) were measured in 86 children in a malaria-holoendemic area of Kenya. The children were then monitored for episodes of clinical malaria for 52 weeks.RESULTS: Children with high levels of IgG antibodies to CSP, LSA-1, and TRAP had a decreased risk of clinical malaria (adjusted hazard ratio, 0.29; 95% confidence interval 0.10-0.81; P = .02), a lower incidence of clinical malaria (P=.006), protection from clinical malaria with a parasite level of \u3e or =4000 parasites/microL (P= .03), and a higher hemoglobin level at enrollment (P= .009), compared with children with lower antibody levels. Protection against malaria morbidity was associated primarily with antibodies to CSP and LSA-1.CONCLUSIONS: Kenyan children with high levels of IgG antibodies to the pre-erythrocytic antigens CSP, LSA-1, and TRAP have a lower risk of developing clinical malaria than children without high levels of these antibodies. The decreased risk of clinical malaria may be mediated in part by prevention of high-density parasitemia.
机译:背景:针对促红细胞生成前抗原的IgG抗体可在疟疾动物模型中预防感染和疾病,但并未与针对人类疟疾的保护相关联。方法:针对环子孢子蛋白(CSP),肝脏-在肯尼亚的疟疾高发区,对86名儿童进行了1期抗原1型(LSA-1)和血小板反应蛋白相关粘附蛋白(TRAP)的检测。结果,对这些儿童进行了52周的临床疟疾监测。结果:患CSP,LSA-1和TRAP的IgG抗体水平高的儿童患疟疾的风险降低(风险比经调整为0.29; 95%的置信区间0.10-0.81; P = .02),临床疟疾发病率较低(P = .006),寄生虫水平为\ u3e或= 4000寄生虫/ microL(P = .03)的对临床疟疾的防护程度较高与抗体水平较低的儿童相比,入院时的血红蛋白水平(P = .009)。结论:肯尼亚儿童对红细胞前抗原CSP,LSA-1和TRAP的IgG抗体含量高,其患疟疾的风险要比儿童低。没有高水平的这些抗体。临床疟疾风险的降低可能部分由预防高密度寄生虫病引起。

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