人类 CAZyme 基因的功能变异与肠易激综合征患者限制碳水化合物饮食疗效的关系。

IF 11.6 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Andreea Zamfir-Taranu, Britt-Sabina Löscher, Florencia Carbone, Abdullah Hoter, Cristina Esteban Blanco, Isotta Bozzarelli, Leire Torices, Karen Routhiaux, Karen Van den Houte, Ferdinando Bonfiglio, Gabriele Mayr, Maura Corsetti, Hassan Y Naim, Andre Franke, Jan Tack, Mauro D'Amato
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引用次数: 0

摘要

背景和目的:限制某些碳水化合物的膳食摄入量对部分肠易激综合征(IBS)患者有治疗效果,但并非所有患者都有这种效果。我们在 DOMINO 研究中调查了人类碳水化合物活性酶(hCAZymes)基因的遗传变异与降低 FODMAP 饮食反应的关系。方法:通过对 6 个感兴趣的基因(AMY2B、LCT、MGAM、MGAM2、SI 和 TREH)进行靶向测序,研究了 DOMINO 试验饮食组(FODMAP-lowering;N=196)和药物组(otilonium bromide;N=54)肠易激综合征患者的 HCAZy 多态性。在累积分析中,将肠易激综合征患者分为携带者组和非携带者组(将所有 hCAZyme 低倍变异体归入一个单独的分区),使用年龄和性别调整的逻辑回归来检验 hCAZyme 多态性。还对hCAZyme变异进行了定量分析,其中考虑了受低形变影响的hCAZyme基因数量:结果:在饮食治疗组中,hCAZyme基因低形变的数量与治疗反应率呈正相关(P=.03,OR=1.51 [CI=0.99-2.32])。在 IBS-D 组(55 人)中,hCAZyme 基因携带者对饮食治疗产生反应的几率是非携带者的六倍(P=.002,OR=6.33 [CI=1.83-24.77])。这些趋势在药物治疗组中没有观察到:结论:HCAZYme 基因变异可能与降低碳水化合物饮食的效果有关。结论:HCAZYme 基因变异可能与降低碳水化合物饮食的疗效有关,这就需要对研究结果进行更多的测试和复制,包括对这一现象的机理进行研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Functional Variation in Human CAZyme Genes in Relation to the Efficacy of a Carbohydrate-Restricted Diet in IBS Patients.

Background & aims: Limiting the dietary intake of certain carbohydrates has therapeutic effects in some but not all irritable bowel syndrome (IBS) patients. We investigated genetic variation in human Carbohydrate-Active enZYmes (hCAZymes) genes in relationship to the response to a FODMAP-lowering diet in the DOMINO study.

Methods: hCAZy polymorphism was studied in patients with IBS from the dietary (FODMAP-lowering; n = 196) and medication (otilonium bromide; n = 54) arms of the DOMINO trial via targeted sequencing of 6 genes of interest (AMY2B, LCT, MGAM, MGAM2, SI, and TREH). hCAZyme defective (hypomorphic) variants were identified via computational annotation using clinical pathogenicity classifiers. Age- and sex-adjusted logistic regression was used to test hCAZyme polymorphisms in cumulative analyses where IBS patients were stratified into carrier and non-carrier groups (collapsing all hCAZyme hypomorphic variants into a single bin). Quantitative analysis of hCAZyme variation was also performed, in which the number of hCAZyme genes affected by a hypomorphic variant was taken into account.

Results: In the dietary arm, the number of hypomorphic hCAZyme genes positively correlated with treatment response rate (P = .03; odds ratio = 1.51; confidence interval = 0.99-2.32). In the IBS-D group (n = 55), hCAZyme carriers were 6 times more likely to respond to the diet than non-carriers (P = .002; odds ratio = 6.33; confidence interval = 1.83-24.77). These trends were not observed in the medication arm.

Conclusions: hCAZYme genetic variation may be relevant to the efficacy of a carbohydrate-lowering diet. This warrants additional testing and replication of findings, including mechanistic investigations of this phenomenon.

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来源期刊
CiteScore
16.90
自引率
4.80%
发文量
903
审稿时长
22 days
期刊介绍: Clinical Gastroenterology and Hepatology (CGH) is dedicated to offering readers a comprehensive exploration of themes in clinical gastroenterology and hepatology. Encompassing diagnostic, endoscopic, interventional, and therapeutic advances, the journal covers areas such as cancer, inflammatory diseases, functional gastrointestinal disorders, nutrition, absorption, and secretion. As a peer-reviewed publication, CGH features original articles and scholarly reviews, ensuring immediate relevance to the practice of gastroenterology and hepatology. Beyond peer-reviewed content, the journal includes invited key reviews and articles on endoscopy/practice-based technology, health-care policy, and practice management. Multimedia elements, including images, video abstracts, and podcasts, enhance the reader's experience. CGH remains actively engaged with its audience through updates and commentary shared via platforms such as Facebook and Twitter.
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