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恶性疟原虫:裂殖子入侵配体EBA-175功能活性区域的进一步特征分析

Plasmodium falciparum: further characterization of a functionally active region of the merozoite invasion ligand EBA-175.

作者信息

Sim B K, Carter J M, Deal C D, Holland C, Haynes J D, Gross M

机构信息

Department of Immunology, Walter Reed Army Institute of Research, Washington DC 20307-5100.

出版信息

Exp Parasitol. 1994 May;78(3):259-68. doi: 10.1006/expr.1994.1027.

Abstract

A 42 amino acid peptide, Pf EBA-175 (1062-1103), also called EBA-peptide 4 of the 175-kDa Plasmodium falciparum sialic acid binding protein, a putative merozoite invasion ligand, has been shown to be a target of parasite growth inhibitory antibodies. We expressed and purified a recombinant protein, NS1-Pf EBA-175 (946-1133) which included the 42 amino acid peptide, and compared antibodies induced by immunization with the protein to antibodies raised against the 42 amino acid peptide. Sera from rabbits immunized with the recombinant protein and the synthetic peptide immunoprecipitated authentic EBA-175, and had comparable ELISA titers against peptide Pf EBA-175 (1062-1103). However, IFAT titers against infected erythrocytes and growth inhibitory activity were substantially higher in sera from animals immunized with the 42 amino acid synthetic peptide. Epitope mapping of the 42 amino acid peptide identified a 19 amino acid peptide, Pf EBA-175 (1069-1087), which blocked the ability of antibodies against the 42 amino acid peptide to (1) immunoprecipitate EBA-175, (2) bind to the 42 amino acid peptide in an ELISA, and (3) recognize infected parasites in an IFAT. Sera from rabbits immunized with the 19 amino acid peptide conjugated to KLH had excellent parasite growth inhibitory activity (at 1:5 serum dilution, 49.9 +/- 7.4%, mean +/- SD of three separate assays), but the activity was lower in each of the three assays than that of sera from rabbits immunized with the 42 amino acid peptide (67.8 +/- 24.8%). These data indicate that the activity of antibodies raised against the linear 42 amino acid peptide, Pf EBA-175 (1062-1103) are primarily, if not exclusively, directed against 19 of the 42 amino acids, and identify this region of Pf EBA 175 as a target for vaccine development.

摘要

一种42个氨基酸的肽,Pf EBA - 175(1062 - 1103),也被称为175 kDa恶性疟原虫唾液酸结合蛋白的EBA - 肽4,一种假定的裂殖子入侵配体,已被证明是寄生虫生长抑制抗体的靶点。我们表达并纯化了一种重组蛋白NS1 - Pf EBA - 175(946 - 1133),其包含该42个氨基酸的肽,并将用该蛋白免疫诱导产生的抗体与针对该42个氨基酸肽产生的抗体进行比较。用重组蛋白和合成肽免疫的兔血清免疫沉淀了天然EBA - 175,并且针对肽Pf EBA - 175(1062 - 1103)具有相当的ELISA滴度。然而,用42个氨基酸合成肽免疫的动物血清中,针对感染红细胞的间接荧光抗体试验(IFAT)滴度和生长抑制活性显著更高。对42个氨基酸肽的表位作图鉴定出一个19个氨基酸的肽,Pf EBA - 175(1069 - 1087),其阻断了针对42个氨基酸肽的抗体进行以下操作的能力:(1)免疫沉淀EBA - 175;(2)在ELISA中与42个氨基酸肽结合;(3)在IFAT中识别感染的寄生虫。用与钥孔血蓝蛋白(KLH)偶联的19个氨基酸肽免疫的兔血清具有优异的寄生虫生长抑制活性(在血清稀释度为1:5时,三次独立试验的平均值±标准差为49.9±7.4%),但在这三次试验中的每一次试验中,该活性均低于用42个氨基酸肽免疫的兔血清(67.8±24.8%)。这些数据表明,针对线性42个氨基酸肽Pf EBA - 175(1062 - 1103)产生的抗体活性,如果不是完全的话,主要针对42个氨基酸中的19个氨基酸,并将Pf EBA 175的这个区域确定为疫苗开发的靶点。

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