Apical membrane antigen-1 (AMA1) is a transmembrane protein present on the surface of merozoites that is thought to be involved in the process of parasite invasion of host erythrocytes. Although it is the target of a natural immune response that can inhibit invasion, little is known about the molecular mechanisms by which AMA1 facilitates the invasion process. In an attempt to identify peptides that specifically interact with and block the function of AMA1, a random peptide library displayed on the surface of filamentous phage was panned on recombinant AMA1 from Plasmodium falciparum. Three peptides with affinity for AMA1 were isolated, and characterization of their fine binding specificities indicated that they bind to a similar region on the surface of AMA1. One of these peptides was found to be a potent inhibitor of the invasion of P. falciparum merozoites into human erythrocytes. We propose that this peptide blocks interaction between AMA1 and a ligand on the erythrocyte surface that is involved in a critical step in malarial invasion. The identification and characterization of these peptide inhibitors now permit an evaluation of the essential requirements that are necessary for efficient neutralization of merozoite invasion by blocking AMA1 function.

译文

:顶膜抗原-1(AMA1)是裂殖子表面上存在的跨膜蛋白,被认为与宿主红细胞的寄生虫入侵有关。尽管它是可以抑制侵袭的天然免疫反应的靶标,但对于AMA1促进侵袭过程的分子机制知之甚少。为了鉴定与AMA1特异性相互作用并阻断其功能的肽,将显示在丝状噬菌体表面的随机肽文库淘选自恶性疟原虫的重组AMA1上。分离了对AMA1具有亲和力的三种肽,表征它们的精细结合特异性表明它们结合到AMA1表面的相似区域。发现这些肽之一是恶性疟原虫裂殖子侵入人红细胞的有效抑制剂。我们建议,该肽阻断AMA1和红细胞表面上的配体之间的相互作用,该配体参与了疟疾入侵的关键步骤。这些肽抑制剂的鉴定和表征现在可以评估通过阻断AMA1功能有效中和裂殖子入侵所需的基本要求。

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