单中心 1000 例儿童全外显子测序识别的单基因变异相关炎症性肠病的流行率和临床特征。
Prevalence and Clinical Features of Inflammatory Bowel Diseases Associated With Monogenic Variants, Identified by Whole-Exome Sequencing in 1000 Children at a Single Center.
机构信息
SickKids Inflammatory Bowel Disease Center, The Hospital for Sick Children, Toronto, Ontario, Canada; School of Medicine, Conway Institute, University College Dublin, Dublin, Ireland; Division of Pediatric Gastroenterology, Western University, Children's Hospital, London Health Sciences Centre, London, Ontario, Canada.
SickKids Inflammatory Bowel Disease Center, The Hospital for Sick Children, Toronto, Ontario, Canada.
出版信息
Gastroenterology. 2020 Jun;158(8):2208-2220. doi: 10.1053/j.gastro.2020.02.023. Epub 2020 Feb 19.
BACKGROUND & AIMS: A proportion of infants and young children with inflammatory bowel diseases (IBDs) have subtypes associated with a single gene variant (monogenic IBD). We aimed to determine the prevalence of monogenic disease in a cohort of pediatric patients with IBD.
METHODS
We performed whole-exome sequencing analyses of blood samples from an unselected cohort of 1005 children with IBD, aged 0-18 years (median age at diagnosis, 11.96 years) at a single center in Canada and their family members (2305 samples total). Variants believed to cause IBD were validated using Sanger sequencing. Biopsies from patients were analyzed by immunofluorescence and histochemical analyses.
RESULTS
We identified 40 rare variants associated with 21 monogenic genes among 31 of the 1005 children with IBD (including 5 variants in XIAP, 3 in DOCK8, and 2 each in FOXP3, GUCY2C, and LRBA). These variants occurred in 7.8% of children younger than 6 years and 2.3% of children aged 6-18 years. Of the 17 patients with monogenic Crohn's disease, 35% had abdominal pain, 24% had nonbloody loose stool, 18% had vomiting, 18% had weight loss, and 5% had intermittent bloody loose stool. The 14 patients with monogenic ulcerative colitis or IBD-unclassified received their diagnosis at a younger age, and their most predominant feature was bloody loose stool (78%). Features associated with monogenic IBD, compared to cases of IBD not associated with a single variant, were age of onset younger than 2 years (odds ratio [OR], 6.30; P = .020), family history of autoimmune disease (OR, 5.12; P = .002), extra-intestinal manifestations (OR, 15.36; P < .0001), and surgery (OR, 3.42; P = .042). Seventeen patients had variants in genes that could be corrected with allogeneic hematopoietic stem cell transplantation.
CONCLUSIONS
In whole-exome sequencing analyses of more than 1000 children with IBD at a single center, we found that 3% had rare variants in genes previously associated with pediatric IBD. These were associated with different IBD phenotypes, and 1% of the patients had variants that could be potentially corrected with allogeneic hematopoietic stem cell transplantation. Monogenic IBD is rare, but should be considered in analysis of all patients with pediatric onset of IBD.
背景与目的
一部分炎症性肠病(IBD)患儿的亚型与单一基因突变有关(单基因 IBD)。本研究旨在确定单基因疾病在儿科 IBD 患者队列中的流行率。
方法
我们对加拿大一家中心的 1005 名年龄 0-18 岁(诊断时的中位年龄为 11.96 岁)的 IBD 患儿及其家庭成员(共 2305 个样本)的未选择的队列的血液样本进行了全外显子组测序分析。使用 Sanger 测序验证了被认为导致 IBD 的变异。对患者的活检进行免疫荧光和组织化学分析。
结果
我们在 1005 名 IBD 患儿中的 31 名中发现了 40 个与 21 个单基因基因相关的罕见变异(包括 XIAP 中的 5 个变异、DOCK8 中的 3 个变异以及 FOXP3、GUCY2C 和 LRBA 中的每个 2 个变异)。这些变异发生在 7.8%的 6 岁以下儿童和 2.3%的 6-18 岁儿童中。在 17 名患有单基因克罗恩病的患者中,35%有腹痛,24%有非血性稀便,18%有呕吐,18%有体重减轻,5%有间歇性血性稀便。14 名患有单基因溃疡性结肠炎或 IBD 未分类的患者的诊断年龄较小,最主要的特征是血性稀便(78%)。与非单一变异相关的 IBD 病例相比,与单基因 IBD 相关的特征为发病年龄小于 2 岁(比值比 [OR],6.30;P =.020)、自身免疫性疾病家族史(OR,5.12;P =.002)、肠外表现(OR,15.36;P <.0001)和手术(OR,3.42;P =.042)。17 名患者的基因变异可通过异基因造血干细胞移植纠正。
结论
在对一家中心的 1000 多名 IBD 患儿进行的全外显子组测序分析中,我们发现 3%的患儿存在先前与儿科 IBD 相关的基因罕见变异。这些变异与不同的 IBD 表型相关,1%的患者的变异可通过异基因造血干细胞移植进行潜在纠正。单基因 IBD 很少见,但应考虑对所有儿科发病的 IBD 患者进行分析。
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