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Synthetic GPI as a candidate antitoxic vaccine in a model of malaria

机译:合成GPI作为疟疾模型中的候选抗毒疫苗

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The malaria parasite Plasmodium falciparum infects 5-10% of the world's population and kills two million people annually. Fatalities are thought to result in part from pathological reactions initiated by a malarial toxin. Glycosylphosphatidylinositol (GPI) originating from the parasite has the properties predicted of a toxin; however, a requirement for toxins in general and GPI in particular in malarial pathogenesis and fatality remains unproven. As anti-toxic vaccines can be highly effective public health tools, we sought to determine whether anti-GPI vaccination could prevent pathology and fatalities in the Plasmodium berghei/rodent model of severe malaria. The P. falciparum GPI glycan of the sequence NH_2-CH_2-CH_2-PO_4-(Manαl-2)6Manαl-2Manα1 -6Manα1 -4GlcNH_2α1 -6myo-inositol-1,2-cyclic-phos-phate was chemically synthesized, conjugated to carriers, and used to immunize mice. Recipients were substantially protected against malarial acidosis, pulmonary oedema, cerebral syndrome and fatality. Anti-GPI antibodies neutralized pro-inflammatory activity by P. falciparum in vitro. Thus, we show that GPI is a significant pro-inflammatory endotoxin of parasitic origin, and that several disease parameters in malarious mice are toxin-dependent. GPI may contribute to pathogenesis and fatalities in humans. Synthetic GPI is therefore a prototype carbohydrate anti-toxic vaccine against malaria.
机译:疟原虫恶性疟原虫感染世界人口的5-10%,每年造成200万人死亡。人们认为死亡的部分原因是由疟疾毒素引发的病理反应。源自寄生虫的糖基磷脂酰肌醇(GPI)具有预测的毒素特性;然而,对毒素的一般要求,尤其是在疟疾的发病机理和致死性方面,尤其是GPI的毒素要求尚未得到证实。由于抗毒性疫苗可以作为高效的公共卫生工具,因此我们试图确定抗GPI疫苗是否可以预防严重疟疾的伯氏疟原虫/啮齿动物模型中的病理学和致死性。化学合成序列NH_2-CH_2-CH_2-PO_4-(Manα1-2-2)6Manα1-2Manα1-6Manα1-4-GlcNH_2α1-6myo-inositol-1,2-cyclic-phos-phate的恶性疟原虫GPI聚糖,并用于免疫小鼠。收件人得到了充分的保护,可以预防疟疾酸中毒,肺水肿,脑综合征和死亡。抗GPI抗体在体外中和了恶性疟原虫的促炎活性。因此,我们表明GPI是寄生虫起源的重要的促炎性内毒素,并且疟疾小鼠中的几种疾病参数都是毒素依赖性的。 GPI可能有助于人类发病和致死。因此,合成GPI是抗疟疾的原型碳水化合物抗毒疫苗。

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