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Innate immunity in ocular Chlamydia trachomatis infection: contribution of IL8 and CSF2 gene variants to risk of trachomatous scarring in Gambians.

机译:眼沙眼衣原体感染的先天免疫:IL8和CSF2基因变异对冈比亚人发生沙眼性疤痕的风险的影响。

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摘要

BACKGROUND: Trachoma, a chronic keratoconjunctivitis caused by Chlamydia trachomatis, is the world's commonest infectious cause of blindness. Blindness is due to progressive scarring of the conjunctiva (trachomatous scarring) leading to in-turning of eyelashes (trichiasis) and corneal opacification. We evaluated the contribution of genetic variation across the chemokine and cytokine clusters in chromosomes 4q and 5q31 respectively to risk of scarring trachoma and trichiasis in a large case-control association study in a Gambian population. METHODS: Linkage disequilibrium (LD) mapping was used to investigate risk effects across the 4q and 5q31 cytokine clusters in relation to the risk of scarring sequelae of ocular Ct infection. Disease association and epistatic effects were assessed in a population based study of 651 case-control pairs by conditional logistic regression (CLR) analyses. RESULTS: LD mapping suggested that genetic effects on risk within these regions mapped to the pro-inflammatory innate immune genes interleukin 8 (IL8) and granulocyte-macrophage colony stimulatory factor (CSF2) loci. The IL8-251 rare allele (IL8-251 TT) was associated with protection from scarring trachoma (OR = 0.29 p = 0.027). The intronic CSF2_27348 A allele in chromosome 5q31 was associated with dose dependent protection from trichiasis, with each copy of the allele reducing risk by 37% (p = 0.005). There was evidence of epistasis, with effects at IL8 and CSF2 loci interacting with those previously reported at the MMP9 locus, a gene acting downstream to IL8 and CSF2 in the inflammatory cascade. CONCLUSION: innate immune response SNP-haplotypes are linked to ocular Ct sequelae. This work illustrates the first example of epistatic effects of two genes on trachoma.
机译:背景:沙眼是由沙眼衣原体引起的一种慢性角膜结膜炎,是世界上最常见的致盲性传染病。失明是由于结膜的渐进性瘢痕形成(气管瘢痕形成),导致睫毛内陷(倒睫)和角膜混浊。在冈比亚人群的大型病例对照研究中,我们分别评估了染色体4q和5q31上趋化因子和细胞因子簇的遗传变异对疤痕性沙眼和倒睫的风险的贡献。方法:采用连锁不平衡(LD)作图法研究了4q和5q31细胞因子簇中与眼部Ct留下疤痕后遗症风险有关的风险影响。通过条件对数回归(CLR)分析,在基于651个病例对照对的人群研究中评估了疾病关联和上位效应。结果:LD图谱表明这些区域内的遗传风险风险映射到促炎先天免疫基因白介素8(IL8)和粒细胞-巨噬细胞集落刺激因子(CSF2)基因座。 IL8-251稀有等位基因(IL8-251 TT)与防止疤痕性沙眼相关(OR = 0.29 p = 0.027)。染色体5q31中的内含子CSF2_27348 A等位基因与针对剂量的对倒睫的保护作用相关,每拷贝等位基因可使患病风险降低37%(p = 0.005)。有上皮证据,对IL8和CSF2基因座的作用与先前在MMP9基因座上报道的作用相互作用,该基因在炎症级联反应中作用于IL8和CSF2的下游。结论:先天性免疫应答SNP单倍型与眼Ct后遗症有关。这项工作说明了两个基因对沙眼的上位性作用的第一个例子。

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