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合成疟疾肽疫苗在特定HLA基因型的疫苗接种者中引发高水平抗体。

Synthetic malaria peptide vaccine elicits high levels of antibodies in vaccinees of defined HLA genotypes.

作者信息

Nardin E H, Oliveira G A, Calvo-Calle J M, Castro Z R, Nussenzweig R S, Schmeckpeper B, Hall B F, Diggs C, Bodison S, Edelman R

机构信息

New York University School of Medicine, Dept. of Medical and Molecular Parasitology, New York, NY 10010, USA.

出版信息

J Infect Dis. 2000 Nov;182(5):1486-96. doi: 10.1086/315871. Epub 2000 Oct 9.

Abstract

A multiple antigen peptide (MAP) malaria vaccine containing minimal Plasmodium falciparum circumsporozoite protein repeat epitopes was assessed for safety and immunogenicity in volunteers of known class II genotypes. The MAP/alum/QS-21 vaccine formulation elicited high levels of parasite-specific antibodies in 10 of 12 volunteers expressing DQB10603, DRB10401, or DRB1*1101 class II molecules. In contrast, volunteers of other HLA genotypes were low responders or nonresponders. A second study of 7 volunteers confirmed the correlation of class II genotype and high responder phenotype. This is the first demonstration in humans that a peptide vaccine containing minimal T and B cell epitopes composed of only 5 amino acids (N, A, V, D, and P) can elicit antibody titers comparable to multiple exposures to irradiated P. falciparum-infected mosquitoes. Moreover, the high-responder phenotypes were predicted by analysis of peptide/HLA interactions in vitro, thus facilitating the rational design of epitope-based peptide vaccines for malaria, as well as for other pathogens.

摘要

一种包含最少恶性疟原虫环子孢子蛋白重复表位的多抗原肽(MAP)疟疾疫苗,在已知II类基因型的志愿者中进行了安全性和免疫原性评估。MAP/明矾/QS-21疫苗配方在12名表达DQB10603、DRB10401或DRB1*1101 II类分子的志愿者中的10名中引发了高水平的寄生虫特异性抗体。相比之下,其他HLA基因型的志愿者是低反应者或无反应者。一项对7名志愿者的第二项研究证实了II类基因型与高反应者表型之间的相关性。这是首次在人体中证明,一种仅由5个氨基酸(N、A、V、D和P)组成的包含最少T细胞和B细胞表位的肽疫苗能够引发与多次暴露于经辐照的感染恶性疟原虫的蚊子相当的抗体滴度。此外,通过体外肽/HLA相互作用分析可以预测高反应者表型,从而有助于合理设计基于表位的疟疾肽疫苗以及针对其他病原体的疫苗。

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