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恶性疟原虫感染期间的疟疾抗原特异性T细胞反应性。

Malaria antigen-specific T-cell responsiveness during infection with Plasmodium falciparum.

作者信息

Wyler D J, Brown J

出版信息

Clin Exp Immunol. 1977 Sep;29(3):401-7.

Abstract

Protective immunity against Plasmodium falciparum develops only after several years of repeated exposure to the malarial parasite. We therefore investigated the possibility that acute malaria was associated with malarial antigen-specific immunosuppression. Peripheral lymphocytes of West Africans with and without P. falciparum infections were tested for their in vitro proliferative responses to a preparation of P. falciparum antigen. There was no significant difference between the magnitude of the proliferative response of lymphocytes from infected as compared to normal Africans, although the responses from both African groups were significantly higher than responses from a group of European controls. Furthermore, no soluble inhibitor of antigen-specific proliferation was present in plasma of infected patients. These observations strongly suggest that if the sluggish development of protective immunity in malaria is based upon infection-related immunosuppression, this occurs without affecting the proliferative responsiveness of specific sensitized, circulating T cells. Preliminary observations also indicate that Europeans residing in Africa and taking malaria prophylaxis may acquire sensitized T cells without experiencing clinically apparent infections.

摘要

针对恶性疟原虫的保护性免疫只有在数年反复接触疟原虫之后才会产生。因此,我们研究了急性疟疾与疟原虫抗原特异性免疫抑制相关的可能性。检测了有和没有恶性疟原虫感染的西非人的外周淋巴细胞对恶性疟原虫抗原制剂的体外增殖反应。与正常非洲人相比,感染非洲人的淋巴细胞增殖反应幅度没有显著差异,尽管这两组非洲人的反应均显著高于一组欧洲对照者的反应。此外,感染患者的血浆中不存在抗原特异性增殖的可溶性抑制剂。这些观察结果强烈表明,如果疟疾中保护性免疫的缓慢发展基于感染相关的免疫抑制,那么这种情况的发生并不影响特异性致敏循环T细胞的增殖反应性。初步观察还表明,居住在非洲并采取疟疾预防措施的欧洲人可能会在没有经历临床明显感染的情况下获得致敏T细胞。

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Malaria: immunity, vaccination and immunodiagnosis.疟疾:免疫、疫苗接种与免疫诊断
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