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重组腺病毒单剂量免疫能有效诱导 CD8+ T 细胞介导的抗疟疾保护性免疫。

Single immunizing dose of recombinant adenovirus efficiently induces CD8+ T cell-mediated protective immunity against malaria.

作者信息

Rodrigues E G, Zavala F, Eichinger D, Wilson J M, Tsuji M

机构信息

Department of Medical and Molecular Parasitology, New York University School of Medicine, New York, NY 10010, USA.

出版信息

J Immunol. 1997 Feb 1;158(3):1268-74.

PMID:9013969
Abstract

The immunogenicity of a recombinant replication defective adenovirus expressing a major malaria Ag, the circumsporozoite (CS) protein (AdPyCS), was determined using a rodent malaria model. A single immunizing dose of this construct induced a large number of CS-specific CD8+ and CD4+ T cells in the spleens of these animals, particularly when given by the s.c. or i.m. route. A single dose of AdPyCS also induced high titers of Abs to Plasmodium yoelii sporozoites in mice. No other form of presentation of the CS protein given as a single immunizing dose, i.e., irradiated sporozoites, recombinant vaccinia, or influenza virus, etc., elicits comparably high numbers of CS-specific CD8+ T cells. The high concentration of CS-specific CD8+ T cells in the spleen was relatively short-lived, decreasing to half of its original value by 4 wk and to one-third at 8 wk after AdPyCS inoculation. The decrease in splenic CS-specific CD4+ T cells was even more rapid. Most importantly, a single dose of inoculation of AdPyCS into mice rendered them highly resistant to sporozoite challenge, resulting in a 93% inhibition of liver stage development of the parasites. This protective effect was primarily mediated by CD8+ T cells, as shown by depletion of this T cell population, while depletion of the CD4+ T cell population had only a minor effect on anti-plasmodial activity. Moreover, the inoculation of mice with AdPyCS induces sterile immunity in a significant proportion of mice, preventing the occurrence of parasitemia.

摘要

使用啮齿动物疟疾模型确定了表达主要疟疾抗原环子孢子(CS)蛋白的重组复制缺陷型腺病毒(AdPyCS)的免疫原性。单次免疫剂量的这种构建体在这些动物的脾脏中诱导产生了大量CS特异性CD8⁺和CD4⁺T细胞,尤其是通过皮下或肌肉注射途径给药时。单次剂量的AdPyCS还在小鼠中诱导产生了高滴度的抗约氏疟原虫子孢子抗体。作为单次免疫剂量给予的CS蛋白的其他任何形式,即辐照子孢子、重组痘苗病毒或流感病毒等,都不会引发数量相当多的CS特异性CD8⁺T细胞。脾脏中高浓度的CS特异性CD8⁺T细胞寿命相对较短,在接种AdPyCS后4周降至其初始值的一半,8周时降至三分之一。脾脏中CS特异性CD4⁺T细胞的减少甚至更快。最重要的是,向小鼠单次接种AdPyCS使它们对子孢子攻击具有高度抗性,导致寄生虫肝期发育受到93%的抑制。如该T细胞群体的耗竭所示,这种保护作用主要由CD8⁺T细胞介导,而CD4⁺T细胞群体的耗竭对抗疟活性只有轻微影响。此外,用AdPyCS接种小鼠在相当比例的小鼠中诱导产生了无菌免疫,防止了寄生虫血症的发生。

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