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接种疟疾疫苗的小鼠的细胞介导免疫

Cell-mediated immunity in mice vaccinated against malaria.

作者信息

Cottrell B J, Playfair J H, De Souza B J

出版信息

Clin Exp Immunol. 1978 Nov;34(2):147-58.

Abstract

Mice vaccinated with a formalin-fixed preparation of either Plasmodium berghei or P. yoelli exhibited delayed type hypersensitivity (DTH) to the homologous antigen. This manifested itself in increased delayed thickening of antigen-challenged pinnae of the vaccinated mice as compared to the non-vaccinated controls. DTH was also evident in the vaccinated mice using the homing of radio-labelled bone marrow cells (BMC) to the delayed lesion as a criterion of reactivity. When P. yoelii vaccinated mice were given a live infection P. yoelii, a marked migration of BMC into the spleen occurred, with a peak at 48 hr, and it is suggested that this was a systemic response of DTH. The splenic T-cells of P. yoelii-vaccinated animals transformed in vitro with a soluble extract of the homologous parasite. The potential function of cell-mediated mechanisms in immunity to malarial infections is discussed.

摘要

用福尔马林固定的伯氏疟原虫或约氏疟原虫制剂免疫的小鼠,对同源抗原表现出迟发型超敏反应(DTH)。与未免疫的对照相比,这表现为免疫小鼠抗原攻击耳廓的迟发性增厚增加。以放射性标记的骨髓细胞(BMC)归巢到迟发性病变作为反应性标准,DTH在免疫小鼠中也很明显。当给约氏疟原虫免疫的小鼠接种活的约氏疟原虫时,BMC显著迁移到脾脏,在48小时达到峰值,提示这是DTH的全身反应。约氏疟原虫免疫动物的脾脏T细胞在体外被同源寄生虫的可溶性提取物转化。讨论了细胞介导机制在疟疾感染免疫中的潜在作用。

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