Olivera Pablo A, Martinez-Lozano Helena, Leibovitzh Haim, Xue Mingyue, Neustaeter Anna, Espin-Garcia Osvaldo, Xu Wei, Madsen Karen L, Guttman David S, Bernstein Charles N, Yerushalmi Baruch, Hyams Jeffrey S, Abreu Maria T, Marshall John K, Wrobel Iwona, Mack David R, Jacobson Kevan, Bitton Alain, Aumais Guy, Panacionne Remo, Dieleman Levinus A, Silverberg Mark S, Steinhart A Hillary, Moayyedi Paul, Turner Dan, Griffiths Anne M, Turpin Williams, Lee Sun-Ho, Croitoru Kenneth
Zane Cohen Centre for Digestive Diseases, Lunenfeld Tanenbaum Research Institute, Mount Sinai Hospital, Toronto, Ontario, Canada; Division of Gastroenterology & Hepatology, University of Toronto Temerty Faculty of Medicine, Toronto, Ontario, Canada.
Zane Cohen Centre for Digestive Diseases, Lunenfeld Tanenbaum Research Institute, Mount Sinai Hospital, Toronto, Ontario, Canada; Division of Gastroenterology & Hepatology, University of Toronto Temerty Faculty of Medicine, Toronto, Ontario, Canada; Department of Digestive System Medicine, Hospital General Universitario, Instituto de Investigación Sanitaria Gregorio Marañón, Madrid, Spain.
Gastroenterology. 2025 Jan;168(1):99-110.e2. doi: 10.1053/j.gastro.2024.08.031. Epub 2024 Sep 3.
BACKGROUND & AIMS: Unaffected first-degree relatives (FDRs) from families with ≥2 affected FDRs with Crohn's disease (CD, multiplex families) have a high risk of developing CD, although the underlying mechanisms driving this risk are poorly understood. We aimed to identify differences in biomarkers between FDRs from multiplex vs simplex families and investigate the risk of future CD onset accounting for potential confounders.
We assessed the Crohn's and Colitis Canada Genetic Environmental Microbial cohort of healthy FDRs of patients with CD. Genome-wide CD-polygenic risk scores, urinary fractional excretion of lactulose-to-mannitol ratio, fecal calprotectin (FCP), and fecal 16S ribosomal RNA microbiome were measured at recruitment. Associations between CD multiplex status and baseline biomarkers were determined using generalized estimating equations models. Cox models were used to assess the risk of future CD onset.
There were 4051 participants from simplex families and 334 from CD multiplex families. CD multiplex status was significantly associated with higher baseline FCP (P = .026) but not with baseline CD-polygenic risk scores or the lactulose-to-mannitol ratio. Three bacterial genera were found to be differentially abundant between both groups. CD multiplex status at recruitment was independently associated with an increased risk of developing CD (adjusted hazard ratio, 3.65; 95% confidence interval, 2.18-6.11, P < .001).
Within FDRs of patients with CD, participants from multiplex families had a 3-fold increased risk of CD onset, a higher FCP, and an altered bacterial composition, but not genetic burden or altered gut permeability. These results suggest that putative environmental factors might be enriched in FDRs from multiplex families.
在患有克罗恩病(CD)的家庭中,若有≥2名患病的一级亲属(FDRs)(多重家庭),其未患病的FDRs患CD的风险较高,尽管导致这种风险的潜在机制尚不清楚。我们旨在确定多重家庭与单重家庭的FDRs之间生物标志物的差异,并调查在考虑潜在混杂因素的情况下未来发生CD的风险。
我们评估了加拿大克罗恩病和结肠炎遗传环境微生物队列中CD患者的健康FDRs。在招募时测量全基因组CD多基因风险评分、乳果糖与甘露醇比值的尿分数排泄、粪便钙卫蛋白(FCP)和粪便16S核糖体RNA微生物组。使用广义估计方程模型确定CD多重状态与基线生物标志物之间的关联。使用Cox模型评估未来发生CD的风险。
来自单重家庭的有4051名参与者,来自CD多重家庭的有334名。CD多重状态与较高的基线FCP显著相关(P = 0.026),但与基线CD多基因风险评分或乳果糖与甘露醇比值无关。发现两组之间有三个细菌属的丰度存在差异。招募时的CD多重状态与发生CD的风险增加独立相关(调整后的风险比为3.65;95%置信区间为2.18 - 6.11,P < 0.001)。
在CD患者的FDRs中,来自多重家庭的参与者患CD的风险增加了3倍,FCP较高,细菌组成改变,但遗传负担或肠道通透性未改变。这些结果表明,假定的环境因素可能在多重家庭的FDRs中更为丰富。
