首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Rabbit and human antibodies to a repeated amino acid sequence of a Plasmodium falciparum antigen Pf 155 react with the native protein and inhibit merozoite invasion.
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Rabbit and human antibodies to a repeated amino acid sequence of a Plasmodium falciparum antigen Pf 155 react with the native protein and inhibit merozoite invasion.

机译:兔和人针对恶性疟原虫抗原Pf 155重复氨基酸序列的抗体与天然蛋白发生反应并抑制裂殖子的入侵。

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摘要

The Plasmodium falciparum-derived antigen of Mr 155,000 designated Pf 155, deposited in the membrane of infected erythrocytes, contains at least two blocks of tandemly repeated amino acid sequences. The peptide Glu-Glu-Asn-Val-Glu-His-Asp-Ala, which corresponds to a subunit of a C-terminally located repeat, was synthesized. Rabbits immunized with the octapeptide conjugated with either keyhole limpet hemocyanine or tetanus toxoid formed antibodies against the octapeptide. These antibodies reacted with Pf 155 as detected by immunoblotting or a modified immunofluorescence assay. Sera from humans exposed to P. falciparum also contained antibodies binding to the octapeptide in a dot-blot immunoassay. Their anti-octapeptide titers were correlated with their immunofluorescence titers in the assay detecting Pf 155 and other parasite antigens in the membrane of infected erythrocytes. Human octapeptide-reactive antibodies were isolated on an affinity column with the octapeptide conjugated to bovine serum albumin as ligand. These human antibodies reacted with Pf 155 in immunoblotting and strongly stained the surface of infected erythrocytes in the modified immunofluorescence assay. Approximately 20% of this immunofluorescence activity in a high-titered human serum could be recovered from the octapeptide column, indicating that a significant fraction of these anti-parasite antibodies react with epitopes associated with the octapeptide. Furthermore, the human octapeptide-reactive antibodies very efficiently inhibited merozoite reinvasion into erythrocytes in vitro. Similarly purified rabbit antibodies also significantly inhibited reinvasion. Our results suggest that the C-terminal segment of repeated peptides in Pf 155 is a major antigenic region of the molecule and may contain target sites for protective immunity in P. falciparum malaria.
机译:155,000先生的恶性疟原虫衍生抗原命名为Pf 155,沉积在受感染红细胞的膜中,包含至少两个串联重复的氨基酸序列块。合成对应于C末端定位的重复序列的亚基的肽Glu-Glu-Asn-Val-Glu-His-Asp-Ala。用与匙孔血蓝蛋白或破伤风类毒素缀合的八肽免疫的兔子形成了针对八肽的抗体。如通过免疫印迹或改良的免疫荧光测定法检测到的,这些抗体与Pf 155反应。在斑点印迹免疫测定中,暴露于恶性疟原虫的人的血清也含有与八肽结合的抗体。在检测感染的红细胞膜中的Pf 155和其他寄生虫抗原的测定中,它们的抗八肽滴度与免疫荧光滴度相关。在亲和柱上分离人八肽反应性抗体,该八肽缀合至牛血清白蛋白作为配体。这些人抗体在免疫印迹中与Pf 155反应,并在改良的免疫荧光测定法中强烈染色了受感染的红细胞表面。在高滴度人血清中约有20%的这种免疫荧光活性可以从八肽柱中回收,表明这些抗寄生虫抗体中有很大一部分会与八肽相关的表位反应。此外,人八肽反应性抗体在体外非常有效地抑制了裂殖子再侵入红细胞。类似地,纯化的兔抗体也显着抑制再侵入。我们的结果表明,Pf 155中重复肽的C末端片段是分子的主要抗原区域,可能包含恶性疟原虫疟疾保护性免疫的靶位点。

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