用基因减毒的p52缺陷伯氏疟原虫孢子子免疫可在肝脏诱导长效效应记忆CD8+ T细胞应答。

Bruno Douradinha, Melissa van Dijk, Geert-Jan van Gemert, Shahid M Khan, Chris J Janse, Andy P Waters, Robert W Sauerwein, Adrian Jf Luty, Bruno Silva-Santos, Maria M Mota, Sabrina Epiphanio
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引用次数: 14

摘要

背景:通过γ辐照或基因缺失减毒的孢子体免疫,可以有效地诱导无菌免疫和对疟疾的持久保护。对于辐射减毒孢子子(RAS)免疫的小鼠,已经证明肝内效应记忆CD8+ T细胞对保护至关重要。最近的研究表明,小鼠的遗传减毒寄生虫(GAP)免疫也由肝效应记忆CD8+ T细胞赋予。在这项研究中,我们分析了缺乏P52蛋白的GAP免疫后的效应记忆细胞反应。我们证明,即使在免疫后6个月,p52-GAP孢子子免疫也会导致效应记忆CD8+ T细胞的强烈增加,而没有检测到特异性CD4+效应T细胞的反应。此外,我们发现效应记忆CD8+ T细胞的增加是肝脏特异性的,而不是脾脏或淋巴结。结论:这些结果表明,用柏氏弓形虫p52-GAP免疫小鼠产生的免疫反应与缺乏UIS3或UIS4表达的RAS或GAP诱导的免疫反应相当,并且在肝内效应记忆CD8+ T细胞中起重要作用。了解不同GAP免疫后保护性免疫的介质对进一步开发由遗传减毒孢子虫组成的疫苗具有重要意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Immunization with genetically attenuated P52-deficient Plasmodium berghei sporozoites induces a long-lasting effector memory CD8+ T cell response in the liver.

Background: The induction of sterile immunity and long lasting protection against malaria has been effectively achieved by immunization with sporozoites attenuated by gamma-irradiation or through deletion of genes. For mice immunized with radiation attenuated sporozoites (RAS) it has been shown that intrahepatic effector memory CD8+ T cells are critical for protection. Recent studies have shown that immunization with genetically attenuated parasites (GAP) in mice is also conferred by liver effector memory CD8+ T cells.

Findings: In this study we analysed effector memory cell responses after immunization of GAP that lack the P52 protein. We demonstrate that immunization with p52-GAP sporozoites also results in a strong increase of effector memory CD8+ T cells, even 6 months after immunization, whereas no specific CD4+ effector T cells response could be detected. In addition, we show that the increase of effector memory CD8+ T cells is specific for the liver and not for the spleen or lymph nodes.

Conclusions: These results indicate that immunization of mice with P. berghei p52-GAP results in immune responses that are comparable to those induced by RAS or GAP lacking expression of UIS3 or UIS4, with an important role implicated for intrahepatic effector memory CD8+ T cells. The knowledge of the mediators of protective immunity after immunization with different GAP is important for the further development of vaccines consisting of genetically attenuated sporozoites.

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