极早发型炎症性肠病11例临床特点分析

doi:10.12372/jcp.2023.23e0031

摘要/Abstract

摘要：

目的探讨极早发型炎症性肠病（VEO-IBD）患儿的临床特点、基因诊断结果、治疗及预后。方法回顾性分析2017年1月至2022年10月在消化科收治及确诊的VEO-IBD患儿的临床资料。结果 11例VEO-IBD患儿，男6例、女5例，中位发病年龄16.0（6.0~29.0）月，其中克罗恩病8例，溃疡性结肠炎1例，未分型炎症性肠病2例。临床症状以腹泻（63.6%）、便血（100%）以及腹痛（45.5%）为主，5例患儿合并肛周病变，2例合并肠狭窄。6例行基因检测的VEO-IBD患儿中，2例存在变异，分别为NOD2、IL10RA基因变异。结论 VEO-IBD的临床表现以腹泻、腹痛、便血为主，容易合并肛周病变，治疗预后差，尤其是单基因变异患儿。对VEO-IBD患儿应进行单基因变异检测，早期实施个体化治疗措施。

关键词: 极早发型炎症性肠病, 基因变异, 预后, 儿童

Abstract:

Objective To explore and analyze the clinical characteristics, genetic diagnosis results, treatment, and prognosis of children with very early onset inflammatory bowel disease (VEO-IBD) in China. Methods A retrospective analysis was conducted on the clinical data of VEO-IBD patients admitted and confirmed from January 2017 to October 2022. Results There were 11 children with VEO-IBD, including 6 males and 5 females; Among them, there were 8 cases of Krohn's disease, 1 case of ulcerative colitis, and 2 cases of undifferentiated inflammatory bowel disease. The median age of onset was16(6-29) months. The main clinical symptoms were diarrhea (63.6%), bloody stools (100%), and abdominal pain (45.5%). Five patients had perianal lesions, and two had intestinal stenosis. Among the 6 VEO-IBD patients who completed gene testing, 2 had genetic mutations, specifically mutations in the NOD2 and IL10RA genes. Conclusions The clinical manifestations of VEO-IBD are mainly diarrhea, abdominal pain, and bloody stool, which are easy to be associated with perianal diseases and have poor treatment prognosis especially for children with single gene variation. Single gene mutation detection should be carried out in children with VEO-IBD, and individual treatment measures should be implemented at anearly stage.

Key words: very early-onset inflammatory bowel disease, gene mutation, prognosis, child

郑新国, 杨辉. 极早发型炎症性肠病11例临床特点分析[J]. 临床儿科杂志, 2023, 41(11): 815-819.

ZHENG Xinguo, YANG Hui. Analysis of clinical feature of 11 cases of very early-onset inflammatory bowel disease[J]. Journal of Clinical Pediatrics, 2023, 41(11): 815-819.

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参考文献 16

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项目	VEO-IBD(n=11)	CD(n=8)	UC(n=1)	IBD-U(n=2)
男性[n(%)]	6(54.6)	5(62.5)	0	1(50.0)
发病年龄[M(P₂₅~P₇₅)]/月	16.0(6.0~29.0)	10.5(4.5~21.5)	49	16, 29
诊断年龄[M(P₂₅~P₇₅)]/月	20.0(13.0~56.0)	19.5(10.8~64.3)	52	16, 39
病程[M(P₂₅~P₇₅)]/月	6.0(2.0~10.0)	7.0(2.0~38.5)	3	0, 10
腹痛[n(%)]	5(45.5)	4(50.0)	0	1(50.0)
腹泻[n(%)]	7(63.6)	5(62.5)	1	1(50.0)
便血[n(%)]	11(100)	8(100)	1	2(100)
蛋白质-能量营养不良[n(%)]	2(18.2)	2(25.0)	0	0
生长迟缓[n(%)]	2(18.2)	2(25.0)	0	0
口腔溃疡[n(%)]	3(27.3)	2(25.0)	0	1(100)
发热[n(%)]	1(9.1)	1(12.5)	0	0
肛周疾病[n(%)]	5(45.5)	5(62.5)	0	0
关节疾病[n(%)]	2(18.2)	2(25.0)	0	0
白细胞计数(x±s)×10⁹·L^-1	14.0±4.6	14.1±4.7	-	-
C反应蛋白[M(P₂₅~P₇₅)]/mg·L^-1	14.6(8.0~30.6)	25.0(10.1~48.0)	-	-
血红蛋白(x±s)/g·L^-1	104.6±12.4	101.5±11.3	-	-
血沉[M(P₂₅~P₇₅)]/mm·h^-1	21.0(8.0~38.0)	32.0(22.8~46.3)	-	-
白蛋白(x±s)/g·L^-1	39.4±5.0	37.4±4.2	-	-
钙卫蛋白[M(P₂₅~P₇₅)]/μg·g^-1	1 046.9(884.1~1 428.5)	913.4(894.4~1 214.0)	-	-

患儿	变异基因	核苷酸位点	变异类型	母亲验证	父亲验证
例1	NOD2	c.488G>A(p.S163N)	杂合	野生	杂合
例2	IL10RA	c.456delC(p.A153fs*33)	杂合	杂合	野生
例2	IL10RA	c.301C>T(p.R101W)	杂合	野生	杂合