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恶性疟原虫疫苗候选抗原AMA1的多样性地理结构以及有症状和无症状感染之间的差异

Geographical structure of diversity and differences between symptomatic and asymptomatic infections for Plasmodium falciparum vaccine candidate AMA1.

作者信息

Cortés Alfred, Mellombo Mata, Mueller Ivo, Benet Ariadna, Reeder John C, Anders Robin F

机构信息

Papua New Guinea Institute of Medical Research, MP511, Madang, Papua New Guinea.

出版信息

Infect Immun. 2003 Mar;71(3):1416-26. doi: 10.1128/IAI.71.3.1416-1426.2003.

Abstract

Plasmodium falciparum apical membrane antigen 1 (AMA1) is a prime malaria vaccine candidate. Antigenic diversity within parasite populations is one of the main factors potentially limiting the efficacy of any asexual-stage vaccine, including one based on AMA1. The DNA coding for the most variable region of this antigen, domain I, was sequenced in 168 samples from the Wosera region of Papua New Guinea, including samples from symptomatic and asymptomatic infections. Neutrality tests applied to these sequences provided strong evidence of selective pressure operating on the sequence of ama1 domain I, consistent with AMA1 being a target of protective immunity. Similarly, a peculiar pattern of geographical diversity and the particular substitutions found were suggestive of strong constraints acting on the evolution of AMA1 at the population level, probably as a result of immune pressure. In addition, a strong imbalance between symptomatic and asymptomatic infections was detected in the frequency of particular residues at certain polymorphic positions, pointing to AMA1 as being one of the determinants of the morbidity associated with a particular strain. The information yielded by this study has implications for the design and assessment of AMA1-based vaccines and provides additional data supporting the importance of AMA1 as a malaria vaccine candidate.

摘要

恶性疟原虫顶端膜抗原1(AMA1)是主要的疟疾疫苗候选抗原。寄生虫群体内的抗原多样性是可能限制任何无性阶段疫苗效力的主要因素之一,包括基于AMA1的疫苗。对来自巴布亚新几内亚沃塞拉地区的168个样本(包括有症状和无症状感染的样本)中该抗原最可变区域(结构域I)的DNA进行了测序。对这些序列进行的中性测试有力地证明了ama1结构域I的序列受到选择压力的作用,这与AMA1是保护性免疫的靶点一致。同样,地理多样性的独特模式以及发现的特定替换表明,在群体水平上,AMA1的进化受到强大限制,这可能是免疫压力的结果。此外,在某些多态性位点的特定残基频率上,有症状和无症状感染之间存在强烈失衡,这表明AMA1是与特定菌株相关发病机制的决定因素之一。本研究产生的信息对基于AMA1的疫苗的设计和评估具有启示意义,并提供了额外的数据支持AMA1作为疟疾疫苗候选抗原的重要性。

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