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小鼠对恶性疟原虫环子孢子重复表位无载体合成聚合物的抗体反应受I-Ab限制:对疟疾疫苗的潜在影响。

The antibody response in mice to carrier-free synthetic polymers of Plasmodium falciparum circumsporozoite repetitive epitope is I-Ab-restricted: possible implications for malaria vaccines.

作者信息

Del Giudice G, Cooper J A, Merino J, Verdini A S, Pessi A, Togna A R, Engers H D, Corradin G, Lambert P H

出版信息

J Immunol. 1986 Nov 1;137(9):2952-5.

PMID:3531341
Abstract

The immunogenicity of a novel synthetic peptide consisting of an average of 40 (Asn-Ala-Asn-Pro) repeats of the circumsporozoite protein of Plasmodium falciparum, (NANP)40, was studied in mice without using any carrier proteins. First, high titers of anti-(NANP)40 antibodies could be obtained after immunization of C57BL/6 mice. These antibodies also reacted with an extract of mosquitoes infected with P. falciparum sporozoites. C57BL/6 nu/nu mice did not produce antibodies against (NANP)40. Secondly, when 14 strains of mice with nine different H-2 haplotypes were immunized with (NANP)40 without carrier, only H-2b mice were found to produce anti-(NANP)40 antibodies, whereas all non-H-2b mice were consistently unresponsive. This response was demonstrated to be I-A-linked by using recombinant and mutant mice. I-Ab [B10.A(5R)] mice produced anti-(NANP)40 antibodies as well as H-2b inbred mice. B6CH-2bm12 I-Ab-mutant mice showed only a very low response. Third, the antibody response against (NANP)40 could be induced in nonresponder mice by immunization with the peptide coupled to a carrier protein. In view of the existence of such an exceptional H-2b restriction in the response to sporozoite synthetic peptides in mice, the triggering of peptide-specific T cell responses in humans receiving sporozoite malaria vaccines might be difficult to achieve.

摘要

在不使用任何载体蛋白的情况下,对小鼠体内一种由恶性疟原虫环子孢子蛋白平均40个(天冬酰胺-丙氨酸-天冬酰胺-脯氨酸)重复序列组成的新型合成肽(NANP)40的免疫原性进行了研究。首先,用(NANP)40免疫C57BL/6小鼠后可获得高滴度的抗(NANP)40抗体。这些抗体也与感染恶性疟原虫子孢子的蚊子提取物发生反应。C57BL/6裸鼠不产生针对(NANP)40的抗体。其次,当用无载体的(NANP)40免疫具有9种不同H-2单倍型的14个小鼠品系时,仅发现H-2b小鼠产生抗(NANP)40抗体,而所有非H-2b小鼠始终无反应。通过使用重组和突变小鼠证明这种反应与I-A相关。I-Ab [B10.A(5R)]小鼠与H-2b近交系小鼠一样产生抗(NANP)40抗体。B6CH-2bm12 I-Ab突变小鼠仅表现出非常低的反应。第三,通过用与载体蛋白偶联的肽免疫,可以在无反应小鼠中诱导针对(NANP)40的抗体反应。鉴于小鼠对子孢子合成肽的反应中存在这种特殊的H-2b限制,在接受子孢子疟疾疫苗的人类中触发肽特异性T细胞反应可能难以实现。

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