钠离子依赖性抗坏血酸转运体基因 SLC23A1 多态性与克罗恩病易感性相关。
Polymorphisms in the sodium-dependent ascorbate transporter gene SLC23A1 are associated with susceptibility to Crohn disease.
机构信息
From Human Nutritional Sciences (MAS, ASL, and PE), The Richardson Centre for Functional Foods and Nutraceuticals (MAS, ASL, and PE), the IBD Clinical and Research Centre (CNB), and the Department of Internal Medicine (CNB and HE-G), University of Manitoba, Winnipeg, Canada.
出版信息
Am J Clin Nutr. 2014 Feb;99(2):378-83. doi: 10.3945/ajcn.113.068015. Epub 2013 Nov 27.
BACKGROUND
Crohn disease (CD) and ulcerative colitis (UC) are 2 common inflammatory bowel diseases (IBDs) associated with intestinal inflammation and tissue damage. Oxidative stress is suggested to play a major role in the initiation and progression of IBD. Vitamin C (ascorbate, ascorbic acid) supplementation has reduced oxidative stress in persons with IBD. The role of ascorbate transporters in IBD remains to be determined. SLC23A1 is a major ascorbate transporter in the intestinal tract, and some of its genetic variants have been associated with severely decreased ascorbate transport and lower systemic concentrations.
OBJECTIVE
This study aimed to determine whether common genetic variants in the vitamin C transporter SLC23A1 are associated with the risk of IBD.
DESIGN
Genomic DNA samples from patients with CD (n = 162) and UC (n = 149) from the Manitoba IBD Cohort Study and ethnically matched controls (n = 142) were genotyped for 3 SLC23A1 polymorphisms (rs6596473, rs33972313, and rs10063949) by using TaqMan assays.
RESULTS
Variation at rs10063949 (G allele for heterozygote and homozygote) was associated with increased susceptibility to CD (OR: 2.54; 95% CI: 1.38, 4.66; OR: 4.72; 95% CI: 2.53, 8.81; P < 0.0001; respectively). A strong linkage disequilibrium (LD) was observed across the SLC23A1 region (variation rs6596473 with rs10063949) for CD and UC (D' = 0.94 and 0.96, respectively). The risk alleles confirmed a haplotype (CGG) that is carried more in CD patients (65.3%, P < 0.0001) than in controls (43.5%).
CONCLUSIONS
A genetic variant (rs10063949-G) in the SLC23A1 ascorbate transporter locus was identified and is associated with an increased risk of CD in a white Canadian IBD cohort. The presented evidence that SLC23A1 variations can modulate the risk of CD has implications for understanding ascorbate transport in CD patients and provides a novel opportunity toward individualized nutritional therapy for patients carrying the disease-associated genotype.
背景
克罗恩病(CD)和溃疡性结肠炎(UC)是两种常见的炎症性肠病(IBD),与肠道炎症和组织损伤有关。氧化应激被认为在 IBD 的发生和发展中起主要作用。维生素 C(抗坏血酸,抗坏血酸)补充剂已减少 IBD 患者的氧化应激。抗坏血酸转运体在 IBD 中的作用仍有待确定。SLC23A1 是肠道中主要的抗坏血酸转运体,其某些遗传变异与严重降低的抗坏血酸转运和较低的全身浓度有关。
目的
本研究旨在确定维生素 C 转运体 SLC23A1 中的常见遗传变异是否与 IBD 的风险相关。
设计
来自马尼托巴 IBD 队列研究的 CD(n = 162)和 UC(n = 149)患者以及种族匹配的对照(n = 142)的基因组 DNA 样本通过 TaqMan 分析针对 3 个 SLC23A1 多态性(rs6596473、rs33972313 和 rs10063949)进行了基因分型。
结果
rs10063949(杂合子和纯合子的 G 等位基因)的变异与 CD 的易感性增加相关(OR:2.54;95%CI:1.38,4.66;OR:4.72;95%CI:2.53,8.81;P <0.0001)。在 CD 和 UC 中,SLC23A1 区域(变异 rs6596473 与 rs10063949)观察到强烈的连锁不平衡(LD)(D'=0.94 和 0.96)。风险等位基因证实了一种单倍型(CGG),在 CD 患者中携带更多(65.3%,P <0.0001),而在对照中携带较少(43.5%)。
结论
在一个加拿大白人 IBD 队列中,鉴定出 SLC23A1 抗坏血酸转运体基因座中的一个遗传变异(rs10063949-G)与 CD 风险增加相关。本研究提供的证据表明,SLC23A1 变异可调节 CD 的风险,这对了解 CD 患者的抗坏血酸转运具有重要意义,并为携带疾病相关基因型的患者提供了个性化营养治疗的新机会。
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