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疟疾血清学图谱显示寄生虫抗原多样性与宿主抗体库之间的交点。

A malaria serological map indicating the intersection between parasite antigenic diversity and host antibody repertoires.

机构信息

Department of Biochemistry, Faculty of Medicine and Medical Sciences, Arabian Gulf University (AGU), P.O. Box 26671, Manama, Kingdom of Bahrain.

出版信息

Eur J Clin Microbiol Infect Dis. 2012 Nov;31(11):3117-25. doi: 10.1007/s10096-012-1673-z. Epub 2012 Jun 29.

Abstract

A malaria vaccine targeting Plasmodium falciparum remains a strategic goal for malaria control. If a polyvalent vaccine is to be developed, its subunits would probably be chosen based on immunogenicity (concentration of elicited antibodies) and associations of selected antigens with protection. We propose an additional possible selection criterion for the inclusion of subunit antigens; that is, coordination between elicited antibodies. For the quantitative estimation of this coordination, we developed a malaria serological map (MSM). Construction of the MSM was based on three categories of variables: (i) malaria antigens, (ii) total IgG and IgG subclasses, (iii) different sources of plasma. To validate the MSM, in this study, we used four malaria antigens (AMA1, MSP2-3D7, MSP2-FC27 and Pf332-C231) and re-grouped the plasma samples into five pairs of subsets based on age, gender, residence, HbAS and malaria morbidity in 9 years. The plasma total IgG and IgG subclasses to the test antigens were measured, and the whole material was used for the MSM construction. Most of the variables in the MSM were previously tested and their associations with malaria morbidity are known. The coordination of response to each antigens pair in the MSM was quantified as the correlation rate (CR = overall number of significant correlations/total number of correlations × 100 %). Unexpectedly, the results showed that low CRs were mostly associated with variables linked with malaria protection and the antigen eliciting the least CRs was the one associated with protection. The MSM is, thus, of potential value for vaccine design and understanding of malaria natural immunity.

摘要

一种针对恶性疟原虫的疟疾疫苗仍然是疟疾控制的一个战略目标。如果要开发一种多价疫苗,其亚单位可能会根据免疫原性(所引发抗体的浓度)和选定抗原与保护的关联来选择。我们提出了一个额外的选择标准,即纳入亚单位抗原的标准;即,所引发的抗体之间的协调。为了定量估计这种协调,我们开发了一种疟疾血清图谱(MSM)。MSM 的构建基于三类变量:(i)疟疾抗原,(ii)总 IgG 和 IgG 亚类,(iii)不同来源的血浆。为了验证 MSM,在这项研究中,我们使用了四种疟疾抗原(AMA1、MSP2-3D7、MSP2-FC27 和 Pf332-C231),并根据年龄、性别、居住地、HbAS 和 9 年来的疟疾发病率,将血浆样本重新分为五组亚组。对测试抗原的血浆总 IgG 和 IgG 亚类进行了测量,整个材料用于 MSM 的构建。MSM 中的大多数变量之前都经过了测试,其与疟疾发病率的关联是已知的。MSM 中每个抗原对的反应协调程度用相关率(CR=总显著相关数/总相关数×100%)来量化。出乎意料的是,结果表明,低 CR 主要与与疟疾保护相关的变量相关,而引发 CR 最低的抗原与保护相关。因此,MSM 对于疫苗设计和理解疟疾自然免疫力具有潜在价值。

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