Fowler Elizabeth V, Doecke James, Simms Lisa A, Zhao Zhen Zhen, Webb Penelope M, Hayward Nicholas K, Whiteman David C, Florin Timothy H, Montgomery Grant W, Cavanaugh Juleen A, Radford-Smith Graham L
Inflammatory Bowel Disease Laboratory, Royal Brisbane and Women's Research Foundation, Brisbane, Australia.
Am J Gastroenterol. 2008 Oct;103(10):2519-26. doi: 10.1111/j.1572-0241.2008.02023.x. Epub 2008 Jul 30.
Crohn's disease (CD) and ulcerative colitis (UC) are the two most common forms of inflammatory bowel disease (IBD), representing a significant health-care burden. A variant in the autophagy gene ATG16L1 (T300A) has been newly identified as a CD susceptibility locus by genome-wide association. Our aim was to assess the contribution of T300A in determining disease susceptibility and phenotype in two independent Australian IBD cohorts and explore the relationship between T300A and known CD risk factors (NOD2[nucleotide-binding oligomerization domain containing 2] status and smoking).
In total, 669 CD and 543 UC cases, and 1,244 controls (study 1), 154 CD cases and 420 controls (study 2), and 702 unaffected parents from both groups were genotyped. We conducted case-control and family association analyses, and investigated relationships between T300A and disease subgroups and between NOD2 status and cigarette smoking (CD only).
The strong association between CD and T300A was confirmed (P < 0.001), with a two-fold increase in disease risk associated with the GG genotype (odds ratio [OR] 1.96, 95% confidence interval [CI] 1.49-2.58), while ileal CD risk was almost three-fold (OR 2.73, CI 1.87-4.0). ATG16L1 and NOD2 were found to contribute independently to CD risk. A greater than seven-fold increased CD risk was observed for current smokers with a GG genotype (vs nonsmoking AA genotype; P < 0.001, OR 7.65, CI 4.21-13.91). A significant inverse association was found between T300A and UC (P= 0.002). This was strongest for patients with extensive, severe disease.
We confirm the strong association between T300A and CD, specifically ileal subphenotype, and also report the first strong association of this variant with UC.
克罗恩病(CD)和溃疡性结肠炎(UC)是炎症性肠病(IBD)最常见的两种形式,给医疗保健带来了重大负担。自噬基因ATG16L1的一个变体(T300A)最近通过全基因组关联研究被确定为CD的一个易感位点。我们的目的是评估T300A在两个独立的澳大利亚IBD队列中对疾病易感性和表型的影响,并探讨T300A与已知CD风险因素(NOD2[含核苷酸结合寡聚化结构域2]状态和吸烟)之间的关系。
总共对669例CD患者、543例UC患者以及1244名对照(研究1)、154例CD患者和420名对照(研究2),以及两组的702名未患病父母进行了基因分型。我们进行了病例对照和家系关联分析,并研究了T300A与疾病亚组之间以及NOD2状态与吸烟之间的关系(仅针对CD患者)。
证实了CD与T300A之间存在强关联(P < 0.001),GG基因型与疾病风险增加两倍相关(优势比[OR]1.96,95%置信区间[CI]1.49 - 2.58),而回肠CD风险几乎增加三倍(OR 2.73,CI 1.87 - 4.0)。发现ATG16L1和NOD2对CD风险有独立影响。对于当前吸烟的GG基因型患者,CD风险增加超过七倍(与不吸烟的AA基因型相比;P < 0.001,OR 7.65,CI 4.21 - 13.91)。发现T300A与UC之间存在显著的负相关(P = 0.002)。这在广泛性、重度疾病患者中最为明显。
我们证实了T300A与CD,特别是回肠亚表型之间存在强关联,并且还首次报道了该变体与UC之间存在强关联。
