P1200 克罗恩病患者维生素 D 代谢基因多态性与肛周疾病的相关性研究

D G Ribaldone, C Cafasso, M Antonucci, A Palermiti, G P Caviglia, M Vernero, A D'Avolio, J Cusato
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Among the mechanisms involved in its pathogenesis we recognise local inflammation and intestinal microbiota alteration. Vitamin D (VD) seems to act on these elements. As there are currently no studies on this subject in the literature, the aim of this study is to evaluate the presence of an association between SNPs of genes coding for enzymes, transporters and receptors involved in the VD pathway and the occurrence of pCD in CD patients. Methods The study was carried out on the biological samples of 206 patients with CD, including 34 with pCD, who were followed up at the inflammatory bowel disease clinic in Turin, Italy. Through the use of Real-Time PCR, the genotype distribution of the following genes were assessed: VDR, CYP27B1, CYP24A1, and GC. For the association study, chi-square test was performed with calculation of p value and, when significant, logistic regression and calculation of OR with 95% CI was performed. Results Studying the association between SNPs and the presence of pCD, the following results were obtained: BsmI p=0.0470 and Apal p=0.0251. For BsmI heterozygous genotype there was an OR=2.5 (95% CI 1.2-5.3) of developing perianal disease and p value=0.02, while for ApaI heterozygous there was OR=2.91 (95% CI 1.3-6.6) of presenting pCD, with p value=0.01. Conclusion In the literature, there are several studies examining the association between the heterozygous Aa genotypes of ApaI and Bb genotypes of BsmI and increased inflammatory markers. In addition, some studies suggest that these two genotypes represent a risk factor for some diseases, including multiple myeloma, systemic lupus erythematosus, and mild cognitive disorder. This study demonstrates for the first time an impact of polymorphisms of genes associated with the VD pathway in predicting the onset of pCD. Specifically, the presence of the heterozygous genotype of BsmI and ApaI significantly increases the risk. 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引用次数: 0

摘要

背景 维生素 D(VD)是一种脂溶性维生素,是钙平衡所必需的,在骨骼外发挥作用。维生素 D 通过 CYP2R1 酶在体内进行第一次羟化,再通过 CYP27B1 酶在肾脏进行第二次羟化,从而获得活性维生素 D。VD 通过 VDBP 转运进入血液循环,并结合其 VDR 受体在靶细胞中发挥活性。最后,VD 被肾脏酶 CYP24A1 灭活。肛周疾病(pCD)是 CD 的一种严重表型表现,可表现为肛周瘘管、脓肿、直肠阴道瘘或狭窄。其发病机制包括局部炎症和肠道微生物群改变。维生素 D(VD)似乎对这些因素起作用。由于目前还没有这方面的文献研究,本研究旨在评估参与 VD 通路的酶、转运体和受体编码基因的 SNPs 与 CD 患者 pCD 发生之间是否存在关联。方法 该研究对意大利都灵炎症性肠病诊所随访的 206 名 CD 患者(包括 34 名 pCD 患者)的生物样本进行了分析。通过实时 PCR 技术,对以下基因的基因型分布进行了评估:VDR、CYP27B1、CYP24A1 和 GC。在关联研究中,进行了卡方检验并计算了 p 值,如果显著,则进行了逻辑回归并计算了 OR 和 95% CI。结果 在研究 SNP 与 pCD 存在之间的关联时,得出了以下结果:BsmI p=0.0470,Apal p=0.0251。BsmI 杂合基因型的肛周疾病发病率为 OR=2.5(95% CI 1.2-5.3),P 值=0.02;而 ApaI 杂合基因型的肛周疾病发病率为 OR=2.91(95% CI 1.3-6.6),P 值=0.01。结论 在文献中,有多项研究探讨了 ApaI 的杂合 Aa 基因型和 BsmI 的杂合 Bb 基因型与炎症标志物增加之间的关联。此外,一些研究表明,这两种基因型是某些疾病的风险因素,包括多发性骨髓瘤、系统性红斑狼疮和轻度认知障碍。本研究首次证明了与 VD 通路相关的基因多态性对预测 pCD 发病的影响。具体来说,BsmI 和 ApaI 的杂合基因型会显著增加发病风险。未来的研究需要在不同和更大的患者群中进行,以证实这些数据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
P1200 Study of correlation between polymorphisms of vitamin D metabolism genes and perianal disease in Crohn's disease
Background Vitamin D (VD) is a fat-soluble vitamin essential for calcium homeostasis and that acts at the extraskeletal level. UVB skin exposure allows the synthesis of provitamin D. This undergoes a first hydroxylation in the leaver by the CYP2R1 enzyme and a second hydroxylation in the kidney by the CYP27B1 enzyme: active VD is obtained. VD is transported into the circulation by VDBP and exerts its activity in the target cells binding its VDR receptor. Finally, VD is inactivated by the renal enzyme CYP24A1. Perianal disease (pCD) is a severe phenotypic manifestation of CD that may present as perianal fistula, abscess, recto-vaginal fistula, or stenosis. Among the mechanisms involved in its pathogenesis we recognise local inflammation and intestinal microbiota alteration. Vitamin D (VD) seems to act on these elements. As there are currently no studies on this subject in the literature, the aim of this study is to evaluate the presence of an association between SNPs of genes coding for enzymes, transporters and receptors involved in the VD pathway and the occurrence of pCD in CD patients. Methods The study was carried out on the biological samples of 206 patients with CD, including 34 with pCD, who were followed up at the inflammatory bowel disease clinic in Turin, Italy. Through the use of Real-Time PCR, the genotype distribution of the following genes were assessed: VDR, CYP27B1, CYP24A1, and GC. For the association study, chi-square test was performed with calculation of p value and, when significant, logistic regression and calculation of OR with 95% CI was performed. Results Studying the association between SNPs and the presence of pCD, the following results were obtained: BsmI p=0.0470 and Apal p=0.0251. For BsmI heterozygous genotype there was an OR=2.5 (95% CI 1.2-5.3) of developing perianal disease and p value=0.02, while for ApaI heterozygous there was OR=2.91 (95% CI 1.3-6.6) of presenting pCD, with p value=0.01. Conclusion In the literature, there are several studies examining the association between the heterozygous Aa genotypes of ApaI and Bb genotypes of BsmI and increased inflammatory markers. In addition, some studies suggest that these two genotypes represent a risk factor for some diseases, including multiple myeloma, systemic lupus erythematosus, and mild cognitive disorder. This study demonstrates for the first time an impact of polymorphisms of genes associated with the VD pathway in predicting the onset of pCD. Specifically, the presence of the heterozygous genotype of BsmI and ApaI significantly increases the risk. Future studies need to be performed in different and larger cohorts of patients in order to confirm these data.
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