Shim Jung Ok
Department of Pediatrics, Korea University Guro Hospital, Korea University College of Medicine, Seoul, Korea.
Intest Res. 2019 Jan;17(1):9-16. doi: 10.5217/ir.2018.00130. Epub 2018 Nov 12.
Recent studies on pediatric inflammatory bowel disease (IBD) have revealed that early-onset IBD has distinct phenotypic differences compared with adult-onset IBD. In particular, very early-onset IBD (VEO-IBD) differs in many aspects, including the disease type, location of the lesions, disease behavior, and genetically attributable risks. Neonatal or infantile-onset IBD develops in less than 1% of pediatric patients. Children with infantile-onset IBD have high rates of affected first-degree relatives and severe disease course. The suspicion of a monogenic cause of VEO-IBD was first confirmed by the discovery of mutations in the genes encoding the interleukin 10 (IL-10) receptors that cause impaired IL-10 signaling. Patients with such mutations typically presented with perianal fistulae, shows a poor response to medical management, and require early surgical interventions in the first year of life. To date, 60 monogenic defects have been identified in children with IBD-like phenotypes. The majority of monogenic defects presents before 6 years of age, and many present before 1 year of age. Next generation sequencing could become an important diagnostic tool in children with suspected genetic defects especially in children with VEO-IBD with severe disease phenotypes. VEO-IBD is a phenotypically and genetically distinct disease entity from adult-onset or older pediatric IBD.
近期关于儿童炎症性肠病(IBD)的研究表明,早发型IBD与成人发病的IBD相比具有明显的表型差异。特别是极早发型IBD(VEO-IBD)在许多方面存在差异,包括疾病类型、病变部位、疾病行为和遗传风险因素。新生儿或婴儿期发病的IBD在不到1%的儿科患者中出现。婴儿期发病的IBD患儿一级亲属受累率高且病程严重。VEO-IBD单基因病因的怀疑首先通过发现编码白细胞介素10(IL-10)受体的基因突变得到证实,这些突变导致IL-10信号传导受损。有此类突变的患者通常表现为肛周瘘管,对药物治疗反应不佳,且在生命的第一年需要早期手术干预。迄今为止,在具有IBD样表型的儿童中已鉴定出60种单基因缺陷。大多数单基因缺陷在6岁之前出现,许多在1岁之前出现。下一代测序可能成为疑似遗传缺陷儿童尤其是具有严重疾病表型的VEO-IBD儿童的重要诊断工具。VEO-IBD是一种在表型和遗传上与成人发病或大龄儿童IBD不同的疾病实体。
