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Genetic control of the immune response in mice to a Plasmodium falciparum sporozoite vaccine. Widespread nonresponsiveness to single malaria T epitope in highly repetitive vaccine

机译:小鼠对恶性疟原虫子孢子疫苗免疫反应的遗传控制。高度重复性疫苗中对单个疟疾T表位的广泛无反应

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摘要

Different H-2 congenic strains of mice were immunized with a P. falciparum sporozoite vaccine currently being tested in humans, or with different segments of the vaccine molecule. Specific IgG production or lymph node cell proliferation in response to different antigens was then determined. Only four of seven strains (representing three of eight possible different class II restriction molecules) responded to the vaccine. Of those restriction molecules, only one, I-Ab, was associated with a response to a malaria-encoded T epitope [contained within NP(NANP)3NA], while the other two molecules (E alpha dE beta d and E alpha kE beta s) were associated with a T cell response to a nonmalarial epitope(s) carboxyterminal to the malaria sequence and encoded by a tetracycline resistance gene, read out of frame. If an analogous situation applies in humans, natural boosting by sporozoites will be very restricted. This has serious implications for the effectiveness of the vaccine, since constant high levels of antisporozoite antibodies and possibly antibody-independent T cell effector functions are required for immunity.
机译:用目前正在人类中测试的恶性疟原虫子孢子疫苗或疫苗分子的不同片段免疫不同的H-2同系小鼠。然后确定响应不同抗原的特异性IgG产生或淋巴结细胞增殖。疫苗中有七个菌株中只有四个(代表八个可能的不同II类限制分子中的三个)。在这些限制分子中,只有一个I-Ab与对疟疾编码的T表位[包含在NP(NANP)3NA中]的反应相关,而其他两个分子(E alpha dE beta d和E alpha kE beta s)与T细胞对疟疾序列羧基末端的非疟原性表位的T细胞应答有关,并由四环素抗性基因编码,读框外。如果类似的情况适用于人类,子孢子的自然促进作用将受到很大限制。这对于疫苗的有效性具有严重的意义,因为免疫力需要恒定高水平的抗子孢子抗体以及可能与抗体无关的T细胞效应子功能。

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