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首页> 外文期刊>Malaria Journal >Frequency of RANTES gene polymorphisms and their association with incidence of malaria: a longitudinal study on children in Iganga district, Uganda
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Frequency of RANTES gene polymorphisms and their association with incidence of malaria: a longitudinal study on children in Iganga district, Uganda

机译:RANTES基因多态性的频率及其与疟疾发病率的关系:乌干达伊冈加地区儿童的纵向研究

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Background The severity and outcome of malaria is influenced by host immunity in which chemokines such as Regulated upon Activation, Normal T cell Expressed and Secreted (RANTES) play an important role. Previous studies show that variations in the RANTES gene affect RANTES protein production, hence altering host immunity. In this study, the relationship between presence of mutations in RANTES and incidence of malaria in a cohort of children living in a malaria-endemic area of Uganda was determined. Methods This was a longitudinal study comprising of 423 children aged between 6 months and 9 years, who were actively followed up for 1 year. Malaria episodes occurring in the cohort children were detected and the affected children treated with national policy drug regimen. Mutations in the RANTES gene were determined by PCR–RFLP method and their frequencies were calculated. A multivariate negative binomial regression model was used to estimate the impact of RANTES mutations on malaria incidence. In all statistical tests, a P-value of <0.05 was considered as significant. Results The frequencies of the ?403A and In1.1C allele were 53.7 and 19.2 %, respectively. No mutations were found at the ?28 locus. After adjustment of incidence rates for age, blood group, insecticide-treated bed net (ITN) use, malaria history and the sickle cell trait, 1n1.1T/C heterozygotes and homozygotes showed a non-significant trend towards higher incidence rates compared to wild-type individuals (IRR = 1.10; P = 0.55 and IRR = 1.25; P = 0.60, respectively). Similarly, there was no significant difference in malaria incidence rates between RANTES ?403G/A heterozygotes or homozygotes and those without mutations (IRR = 1.09; P = 0.66 and IRR = 1.16; P = 0.50, respectively). No relation was seen between RANTES polymorphisms, baseline parasite densities and the time to first re-infection after administration of anti-malaria drugs. Conclusions This study showed that the ?403A mutation occurs in nearly half of the study population and the In1.1C allele occurs in one in every four children. Despite the high frequency of these mutations, there was no clear association with malaria incidence. Other studies evaluating more markers, that could potentially modulate RANTES gene transcription alongside other genetic modifiers of malaria susceptibility, may provide further explanations to these less dramatic findings.
机译:背景技术疟疾的严重程度和结果受宿主免疫力的影响,其中趋化因子(如激活后调控,正常T细胞表达和分泌(RANTES))起着重要作用。先前的研究表明,RANTES基因的变异会影响RANTES蛋白质的产生,从而改变宿主的免疫力。在这项研究中,确定了生活在乌干达疟疾流行地区的一组儿童中RANTES突变的存在与疟疾发生率之间的关系。方法这是一项纵向研究,由423名6个月至9岁的儿童组成,他们接受了1年的积极随访。检测到队列儿童中发生了疟疾发作,并用国家政策药物治疗方案对受影响的儿童进行了治疗。通过PCR-RFLP方法确定RANTES基因的突变,并计算其频率。多元负二项式回归模型用于估计RANTES突变对疟疾发病率的影响。在所有统计测试中,P值<0.05被认为是显着的。结果Δ403A和In1.1C等位基因的频率分别为53.7和19.2%。在〜28位点没有发现突变。调整了年龄,血型,使用杀虫剂处理过的蚊帐(ITN),疟疾史和镰状细胞性状的发病率后,与野生相比,1n1.1T / C杂合子和纯合子的发病率没有显着趋势型个体(IRR = 1.10; P = 0.55和IRR = 1.25; P = 0.60)。同样,RANTES 403G / A杂合子或纯合子与无突变者之间的疟疾发病率也没有显着差异(分别为IRR = 1.09; P = 0.66和IRR = 1.16; P = 0.50)。在服用抗疟疾药物后,RANTES基因多态性,基线寄生虫密度与首次再次感染的时间之间没有关系。结论该研究表明,?403A突变发生在近一半的研究人群中,而In1.1C等位基因发生在每四个孩子中的一个。尽管这些突变的发生频率很高,但与疟疾的发病率没有明确的关联。其他评估更多标记物的研究可能与其他对疟疾易感性的遗传修饰物一起可能调节RANTES基因转录,这些研究可能为这些不太引人注目的发现提供进一步的解释。

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