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No significant impact of IFN-γ pathway gene variants on tuberculosis susceptibility in a West African population

机译:干扰素-γ途径基因变异对西非人群的结核病易感性无明显影响

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摘要

The concept of interferon-γ (IFN-γ) having a central role in cell-mediated immune defence to Mycobacterium tuberculosis has long been proposed. Observations made through early candidate gene studies of constituents of the IFN-γ pathway have identified moderately associated variants associated with resistance or susceptibility to tuberculosis (TB). By analysing 20 major genes whose proteins contribute to IFN-γ signalling we have assessed a large fraction of the variability in genes that might contribute to susceptibility to TB. Genetic variants were identified by sequencing the promoter regions and all exons of IFNG, IFNGR1, IFNGR2, IRF1, IL12A, IL12B, IL12RB1, IL12RB2, IL23A, IL23R, IL27, EBI3, IL27RA, IL6ST, SOCS1, STAT1, STAT4, JAK2, TYK2 and TBX21 in 69 DNA samples from Ghana. In addition, we screened all exons of IFNGR1 in a Ghanaian study group comprising 1999 TB cases and 2589 controls by high-resolution melting point analysis. The fine-mapping approach allows for a detailed screening of all variants, common and rare. Statistical comparisons of cases and controls, however, did not yield significant results after correction for multiple testing with any of the 246 variants selected for genotyping in this investigation. Gene-wise haplotype tests and analysis of rare variants did not reveal any significant association with susceptibility to TB in our investigation as well. Although this analysis was applied on a plausible set of IFN-γ pathway genes in the largest African TB cohort available so far, the lack of significant results challenges the view that genetic marker of the IFN-γ pathway have an important impact on susceptibility to TB.
机译:长期以来提出了在细胞介导的针对结核分枝杆菌的免疫防御中起主要作用的干扰素-γ(IFN-γ)概念。通过对IFN-γ途径的成分进行早期候选基因研究,发现已确定了与结核病(TB)耐药性或易感性相关的中度相关变异。通过分析其蛋白质有助于IFN-γ信号转导的20个主要基因,我们评估了可能导致结核病易感性的基因变异的很大一部分。通过对IFNG,IFNGR1,IFNGR2,IRF1,IL12A,IL12B,IL12RB1,IL12RB2,IL23A,IL23R,IL27,EBI3, IL27RA IL6ST的启动子区域和所有外显子进行测序来鉴定遗传变异 SOCS1 STAT1 STAT4 JAK2 TYK2 和加纳的69个DNA样品中的 TBX21 。此外,我们通过高分辨率熔点分析在加纳研究小组(包括1999 TB病例和2589例对照)中筛选了所有 IFNGR1 外显子。精细映射方法允许详细筛选所有常见和罕见的变体。但是,在对本研究中选择用于基因分型的246个变异中的任何一个进行多重测试校正后,病例和对照的统计学比较未产生明显的结果。在我们的研究中,基因型单倍型测试和罕见变体的分析也没有显示出与结核病易感性的任何显着关联。尽管此分析已应用于迄今为止最大的非洲TB队列中一组可能的IFN- γ通路基因,但缺乏重要结果,这一观点挑战了IFN- 的遗传标记γ途径对结核病易感性有重要影响。

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