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首页> 外文期刊>BMC Infectious Diseases >Effect of hookworm infection and anthelmintic treatment on naturally acquired antibody responses against the GMZ2 malaria vaccine candidate and constituent antigens
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Effect of hookworm infection and anthelmintic treatment on naturally acquired antibody responses against the GMZ2 malaria vaccine candidate and constituent antigens

机译:钩虫感染和αsthelmintic治疗对GMZ2疟疾疫苗候选和组成抗原的天然抗体反应的影响

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Malaria and helminths diseases are co-endemic in most parts of sub-Saharan Africa. Immune responses from each of these pathogens interact, and these interactions may have implications on vaccines. The GMZ2 malaria vaccine candidate is a fusion protein of Plasmodium falciparum merozoite surface protein 3 (MSP3) and glutamate rich protein (GLURP R0). GMZ2 has recently showed modest efficacy in a phase IIb multicenter trial. Here, we assessed the effect of hookworm (Necator americanus) infection and anthelmintic treatment on naturally acquired antibody responses against GMZ2 and constituent antigens. This longitudinal cross-sectional study was conducted in the Kintampo North Municipality of Ghana. Blood and stool samples were taken from 158 individuals (4–88?years old) infected with either P. falciparum alone (n?=?59) or both hookworm and P. falciparum (n?=?63) and uninfected endemic controls (n?=?36). Stool hookworm infection was detected by the Kato-Katz method and PCR. Malaria parasitaemia was detected by RDT, light microscopy and P. falciparum-specific 18S rRNA gene PCR. Serum samples were obtained prior to hookworm treatment with a single dose of albendazole (400?mg) and 3 weeks (21?days) after treatment. Levels of IgG1, IgG3 and IgM against GMZ2, MSP3 and GLURP R0 were measured by ELISA and compared among the groups, before and after treatment. Participants with P. falciparum and hookworm co-infection had significantly higher IgG3 levels to GMZ2 than those with only P. falciparum infection and negative control (p??0.05) at baseline. Treatment with albendazole led to a significant reduction in IgG3 levels against both GMZ2 and GLURP R0. Similarly, IgM and IgG1 levels against MSP3 also decreased following deworming treatment. Individuals with co-infection had higher antibody responses to GMZ2 antigen. Treatment of hookworm/malaria co-infection resulted in a reduction in antibody responses against GMZ2 and constituent antigens after albendazole treatment. Thus, hookworm infection and treatment could have a potential implication on malaria vaccine efficacy.
机译:疟疾和蠕虫在撒哈拉以南非洲的大多数部分都是合作的。来自这些病原体中的每一个相互作用的免疫应答,这些相互作用可能对疫苗有影响。 GMZ2疟疾疫苗候选者是疟原虫疟原虫的融合蛋白,疟原虫疟原虫表面蛋白3(MSP3)和富含谷氨酸富蛋白质(Glurp R0)。 GMZ2最近在IIB MultiCenter试验中显示出适度的功效。在这里,我们评估了钩虫(Necator Americanus)感染和anthelmintic治疗对GMZ2和组成抗原的天然抗体反应的影响。这种纵剖面研究是在加纳的克林德清洗北市进行的。血液和粪便样品从158个个体(4-88岁)仅感染P. falciparum(n?=?59)或钩虫和p. falciparum(n?=Δ63)和未感染的地方控制( n?=?36)。通过Kato-Katz方法和PCR检测粪便钩虫感染。通过RDT,光学显微镜和P. falciParum 18s rRNA基因PCR检测疟疾寄生虫。在治疗后用单剂量的阿贝扎唑(400×Mg)和3周(21℃),获得血清样品。通过ELISA测量对抗GMZ2,MSP3和GLURP R0的IgG1,IgG3和IgM的水平,并在治疗前后进行组。与P.Malciparum和Cokworm Co.Coxware的参与者显着高于GMZ2的IgG3水平明显高于仅在基线上仅具有P.Malciparum感染和阴性对照(P = 0.05)的那些。用阿美唑治疗导致对GMZ2和Glurp R0的IgG3水平显着降低。类似地,随着MSP3的IgM和IgG1水平也降低了以下导虫治疗。具有共感染的个体对GMZ2抗原具有更高的抗体反应。钩虫/疟疾的治疗有助性导致抗体反应对GMZ2和组分抗原的抗体反应减少治疗。因此,钩虫感染和治疗可能对疟疾疫苗疗效产生潜在的含义。

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