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首页> 外文期刊>Malaria Journal >IL1B, IL4R, IL12RB1 and TNF gene polymorphisms are associated with Plasmodium vivax malaria in Brazil
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IL1B, IL4R, IL12RB1 and TNF gene polymorphisms are associated with Plasmodium vivax malaria in Brazil

机译:IL1B,IL4R,IL12RB1和TNF基因多态性与巴西间日疟原虫相关

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Background Malaria is among the most prevalent parasitic diseases worldwide. In Brazil, malaria is concentrated in the northern region, where Plasmodium vivax accounts for 85% disease incidence. The role of genetic factors in host immune system conferring resistance/susceptibility against P. vivax infections is still poorly understood. Methods The present study investigates the influence of polymorphisms in 18 genes related to the immune system in patients with malaria caused by P. vivax. A total of 263 healthy individuals (control group) and 216 individuals infected by P. vivax (malaria group) were genotyped for 33 single nucleotide polymorphisms (SNPs) in IL1B, IL2, IL4, IL4R, IL6, IL8, IL10, IL12A, IL12B, IL12RB1, SP110, TNF, TNFRSF1A, IFNG, IFNGR1, VDR, PTPN22 and P2X7 genes. All subjects were genotyped with 48 ancestry informative insertion-deletion polymorphisms to determine the proportion of African, European and Amerindian ancestry. Only 13 SNPs in 10 genes with differences lower than 20% between cases and controls in a Poisson Regression model with age as covariate were further investigated with a structured population association test. Results The IL1B gene -5839C?>?T and IL4R 1902A?>?G polymorphisms and IL12RB1 -1094A/-641C and TNF -1031 T/-863A/-857 T/-308 G/-238 G haplotypes were associated with malaria susceptibility after population structure correction (p?=?0.04, p?=?0.02, p?=?0.01 and p?=?0.01, respectively). Conclusion Plasmodium vivax malaria pathophysiology is still poorly understood. The present findings reinforce and increase our understanding about the role of the immune system in malaria susceptibility.
机译:背景疟疾是全世界最普遍的寄生虫病之一。在巴西,疟疾集中在北部地区,间日疟原虫占疾病发病率的85%。遗传因素在宿主免疫系统中赋予对间日疟原虫感染的抗性/敏感性的作用仍然知之甚少。方法本研究调查了间日疟原虫引起的疟疾患者中与免疫系统相关的18个基因的多态性。对共263名健康个体(对照组)和216名被间日疟原虫感染的个体(疟疾组)进行了基因分型,分析了IL1B,IL2,IL4,IL4R,IL6,IL8,IL10,IL12A,IL12B中的33个单核苷酸多态性(SNP) ,IL12RB1,SP110,TNF,TNFRSF1A,IFNG,IFNGR1,VDR,PTPN22和P2X7基因。所有受试者均进行了48种祖先信息性插入-缺失多态性的基因分型,以确定非洲,欧洲和美洲印第安人祖先的比例。在带有年龄作为协变量的Poisson回归模型中,病例与对照之间的10个基因中只有13个SNP差异低于20%,采用结构化的群体关联检验。结果IL1B基因-5839Cβ>ΔT和IL4R1902Aβ>ΔG多态性以及IL12RB1-1094A / -641C和TNF-1031T / -863A / -857T / -308G / -238G单倍型与疟疾有关人口结构校正后的敏感性(分别为p?=?0.04,p?=?0.02,p?=?0.01和p?=?0.01)。结论间日疟原虫疟疾的病理生理学仍知之甚少。目前的发现加强和增加了我们对免疫系统在疟疾易感性中的作用的了解。

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