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Restricted or absent immune responses in human populations to Plasmodium falciparum gamete antigens that are targets of malaria transmission-blocking antibodies

机译:人群中对恶性疟原虫配子抗原的限制或缺乏免疫反应,而恶性疟原虫是疟疾传播阻断抗体的靶标

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We have studied the antibodies to sexual stage antigens of Plasmodium falciparum in human sera from Papua New Guinea where intense transmission of P. falciparum occurs as well as the less prevalent P. malariae and P. vivax. In extracts of gametes of P. falciparum we have studied the reactivity of serum antibodies with antigens labeled with 125I on the surface of the gametes as well as intracellular gamete antigens. A prominent 27-kD sexual stage-specific intracellular protein was recognized more or less in proportion to the general antibody response to gamete proteins. The response to the gamete surface proteins, however, was quite unrepresentative of the general antibody response to the intracellular gamete proteins. No antibodies were detected against Pfs25, a 21-kD protein expressed on zygotes and ookinetes of P. falciparum and known to be a sensitive target of malaria transmission-blocking antibodies. The antibody response to two other target antigens of transmission-blocking antibodies on the surface of gametes of P. falciparum, a 230- and a 48- and 45-kD protein doublet, was very variable and independent of the response to the internal protein antigens. Several possibilities are discussed that may account for the variable response to these gamete surface antigens in individuals with otherwise good antibody responses to internal sexual stage proteins. Among these is the possibility that there is MHC restriction of the immune response to the gamete surface antigens in the human population. This interpretation accords well with evidence for MHC-restricted immune response to the same P. falciparum gamete surface antigens in studies with H-2 congenic mice (24).
机译:我们已经研究了来自巴布亚新几内亚的人血清中恶性疟原虫的性阶段抗原的抗体,那里发生了恶性疟原虫的强烈传播,以及疟疾和间日疟原虫的流行较少。在恶性疟原虫的配子提取物中,我们研究了血清抗体与配子表面上标记有125I的抗原以及细胞内配子抗原的反应性。与对配子蛋白的一般抗体反应成比例的或多或少地认识到突出的27 kD有性阶段特异性细胞内蛋白。然而,对配子表面蛋白的反应不能完全代表对细胞内配子蛋白的一般抗体反应。没有检测到针对Pfs25的抗体,Pfs25是一种在恶性疟原虫的受精卵和卵子表达的21-kD蛋白,已知是疟疾传播阻断抗体的敏感靶标。恶性疟原虫配子表面上对传输阻断抗体的其他两种靶抗原的抗体反应是230 k和48 k和45 kD的蛋白质双峰,变化很大,并且与对内部蛋白质抗原的反应无关。讨论了几种可能性,这些可能性可以解释对个体具有对内部性阶段蛋白的良好抗体反应的个体对这些配子表面抗原的可变反应。在这些人群中,可能存在MHC限制人类人群对配子表面抗原的免疫反应。这种解释与在H-2同基因小鼠的研究中针对同一恶性疟原虫配子表面抗原的MHC限制性免疫反应的证据非常吻合(24)。

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