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对来自巴西自然暴露于疟疾的个体的恶性疟原虫环子孢子蛋白中含T和B表位的多种抗原肽的免疫反应。

Immune responses to multiple antigen peptides containing T and B epitopes from Plasmodium falciparum circumsporozoite protein of Brazilian individuals naturally exposed to malaria.

作者信息

Avila S L, Goldberg A C, Arruk V G, Marin M L, Guilherme L, Kalil J, Ferreira A W

机构信息

Institute of Tropical Medicine of São Paulo, School of Medicine, University of São Paulo, Brazil.

出版信息

Parasite Immunol. 2001 Feb;23(2):103-8. doi: 10.1046/j.1365-3024.2001.00363.x.

Abstract

We have evaluated the immune responses of individuals living in a malaria endemic area of Brazil to the (T1B)4, a multiple antigen peptide (MAP) from Plasmodium falciparum circumsporozoite (CS) protein and the related monoepitope MAPs, B4 and (T1)4, and the linear peptides, T1B and B. The highest antibody frequencies were against MAPs containing the B cell epitope sequence (T1B)4 (42.2%) and B4 (28.8%), while the highest lymphoproliferative response frequencies were against the MAPs containing the T cell epitope sequence (T1)4 (47%) and (T1B)4 (36.4%). We analysed individual responses considering lymphoproliferative response to (T1)4 MAP and IgG antibody titre to (T1B)4 as patterns of ideal cellular and humoral responses, respectively. The frequency of responders, cellular and/or humoral was 66.6%, significantly higher than non responders (P = 0.003). We also determined the HLA class II haplotype of each individual but no association between these and immune response patterns to the MAPs was observed. The results showed that individuals primed against P. falciparum in their natural habitat, present a very diverse array of responses against the same peptide antigens, varying from no response in one-third of the individuals to cognate B and T cell responses. Our study underlines the importance of previous studies of vaccine candidates to guarantee that the immunization will be capable of reverting inefficient or absent responses to malaria epitopes.

摘要

我们评估了生活在巴西疟疾流行地区的个体对(T1B)4(一种来自恶性疟原虫环子孢子蛋白(CS)的多抗原肽(MAP))、相关单表位MAP(B4和(T1)4)以及线性肽(T1B和B)的免疫反应。抗体频率最高的是针对含有B细胞表位序列的MAP((T1B)4,42.2%)和B4(28.8%),而淋巴细胞增殖反应频率最高的是针对含有T细胞表位序列的MAP((T1)4,47%)和(T1B)4(36.4%)。我们分别将对(T1)4 MAP的淋巴细胞增殖反应和对(T1B)4的IgG抗体滴度作为理想细胞和体液反应模式,分析个体反应。有细胞和/或体液反应的个体频率为66.6%,显著高于无反应者(P = 0.003)。我们还确定了每个个体的HLA II类单倍型,但未观察到这些单倍型与对MAP的免疫反应模式之间存在关联。结果表明,在自然栖息地接触过恶性疟原虫的个体,对相同肽抗原呈现出非常多样的反应,从三分之一的个体无反应到同源B细胞和T细胞反应不等。我们的研究强调了先前对候选疫苗进行研究的重要性,以确保免疫接种能够扭转对疟疾表位低效或无反应的情况。

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