伯氏疟原虫Hsp90含有啮齿动物和人类疟原虫常见的天然免疫原性I-Ab限制抗原

Q4 Immunology and Microbiology
Matthias H. Enders , Ganchimeg Bayarsaikhan , Sonia Ghilas , Yu Cheng Chua , Rose May , Maria N. de Menezes , Zhengyu Ge , Peck Szee Tan , Anton Cozijnsen , Vanessa Mollard , Katsuyuki Yui , Geoffrey I. McFadden , Mireille H. Lahoud , Irina Caminschi , Anthony W. Purcell , Ralf B. Schittenhelm , Lynette Beattie , William R. Heath , Daniel Fernandez-Ruiz
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引用次数: 7

摘要

深入了解CD4 T细胞在免疫中的作用可以通过对特定特异性反应的研究得到极大的帮助。这需要了解疟原虫衍生的免疫原性表位,其中只有少数已被确定,特别是小鼠C57BL/6背景。我们最近开发了一种TCR转基因小鼠系,称为PbT-II,其产生CD4+ T细胞特异性针对MHC II类(I-Ab)限制性疟原虫表位,并对孢子虫和血期柏氏疟原虫均有反应。在这里,我们鉴定了P. berghei热休克蛋白90中的一个肽,作为PbT-II细胞识别的同源表位。我们发现感染柏氏假体的C57BL/6小鼠可诱导内源性CD4 T细胞对该表位的特异性反应,这表明naïve库中存在与PbT-II细胞相似的特异性细胞。过继转移体外激活的TH1-,特别是th2极化的PbT-II细胞,可改善C57BL/6小鼠对伯氏疟原虫病的控制,并大大减少实验性脑型疟疾的发病。我们的研究结果确定了一个多功能的、潜在的保护性MHC-II限制性表位,可用于探索CD4 T细胞介导的免疫和针对疟疾的疫苗接种策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Plasmodium berghei Hsp90 contains a natural immunogenic I-Ab-restricted antigen common to rodent and human Plasmodium species

Plasmodium berghei Hsp90 contains a natural immunogenic I-Ab-restricted antigen common to rodent and human Plasmodium species

Thorough understanding of the role of CD4 T cells in immunity can be greatly assisted by the study of responses to defined specificities. This requires knowledge of Plasmodium-derived immunogenic epitopes, of which only a few have been identified, especially for the mouse C57BL/6 background. We recently developed a TCR transgenic mouse line, termed PbT-II, that produces CD4+ T cells specific for an MHC class II (I-Ab)-restricted Plasmodium epitope and is responsive to both sporozoites and blood-stage P. berghei. Here, we identify a peptide within the P. berghei heat shock protein 90 as the cognate epitope recognised by PbT-II cells. We show that C57BL/6 mice infected with P. berghei blood-stage induce an endogenous CD4 T cell response specific for this epitope, indicating cells of similar specificity to PbT-II cells are present in the naïve repertoire. Adoptive transfer of in vitro activated TH1-, or particularly TH2-polarised PbT-II cells improved control of P. berghei parasitemia in C57BL/6 mice and drastically reduced the onset of experimental cerebral malaria. Our results identify a versatile, potentially protective MHC-II restricted epitope useful for exploration of CD4 T cell-mediated immunity and vaccination strategies against malaria.

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