首页> 美国卫生研究院文献>The EMBO Journal >Human T cells recognize polymorphic and non-polymorphic regions of the Plasmodium falciparum circumsporozoite protein.
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Human T cells recognize polymorphic and non-polymorphic regions of the Plasmodium falciparum circumsporozoite protein.

机译:人T细胞可识别恶性疟原虫环子孢子蛋白的多态性和非多态性区域。

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摘要

In order to characterize T cell epitopes in the Plasmodium falciparum circumsporozoite (CS) protein sequence, we isolated T cell clones, from non-immune donors, which reacted with synthetic peptides corresponding to two predicted CS protein T cell epitopes. Peptide CS.T3 (corresponding to a non-polymorphic region of the CS protein, residues 378-398) was recognized in association with either DR2 or DRw9 restriction elements. T cell clones recognizing CS.T3 also reacted with the sporozoite-derived CS protein. Peptide CS.T2 corresponds to a polymorphic region (residues 325-341) of the CS protein. Unlike the CS.T3-specific clones, the CS.T2-specific clones did not recognize the CS protein. Since the CS.T2 peptide includes residues which are polymorphic in different P. falciparum isolates, we investigated whether these residues were critical for recognition of the peptide. We show here that a single amino acid substitution at a position of the CS protein which shows genetic polymorphism affects recognition of the sequence by human T cells. The implications of these data for malaria vaccine development are discussed.
机译:为了表征恶性疟原虫环子孢子虫(CS)蛋白序列中的T细胞表位,我们从非免疫供体中分离了T细胞克隆,它们与对应于两个预测的CS蛋白T细胞表位的合成肽反应。与DR2或DRw9限制元件相关联地识别了肽CS.T3(对应于CS蛋白的非多态性区域,残基378-398)。识别CS.T3的T细胞克隆也与子孢子来源的CS蛋白反应。肽CS.T2对应于CS蛋白的多态性区域(残基325-341)。与CS.T3特异性克隆不同,CS.T2特异性克隆无法识别CS蛋白。由于CS.T2肽包含在不同的恶性疟原虫分离物中具有多态性的残基,因此我们研究了这些残基对于识别该肽是否至关重要。我们在这里显示在CS蛋白的位置上显示遗传多态性的单个氨基酸取代会影响人T细胞对该序列的识别。讨论了这些数据对疟疾疫苗开发的影响。

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