[婴儿胆汁淤积症的病因和临床指标分析]。

Q3 Medicine
Q Z Li, C Fan, X S Zhao, Q J Liu, D Qin, P Wang, L Zhu
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引用次数: 0

摘要

目的探讨婴幼儿胆汁淤积症的疾病谱及相应的临床指标,为早期诊断此类疾病提供依据。方法收集2018年1月-2023年3月贵阳市妇幼保健院消化内科诊断为婴幼儿胆汁淤积症的203例住院患儿的临床资料,其中男130例,女73例。入院后回顾性分析患者的一般情况、个人病史以及血液生化检查指标,包括肝功能、凝血功能、血氨、血脂、血糖、TORCH、甲状腺功能等。对部分患者进行了胆管造影和高通量基因测序。对入选病例的病因进行了分析。将儿童的临床数据与不同的遗传代谢性肝病(A 组)和胆道闭锁(B 组)进行比较。根据不同数据采用t检验、Mann-Whitney检验、Kruskal-Wallis检验或χ2检验进行统计分析。结果33例患者的胆汁淤积病因是感染因素,主要是CMV感染。40例患者的胆管发育异常,主要是胆道闭锁、胆总管囊肿和肝内胆管发育不良。26例病例的遗传代谢因素主要包括枸橼酸蛋白缺乏症、钠-头孢胆酸共转运多肽缺乏症和阿拉吉尔综合征。11例有药物/中毒因素(肠外营养相关性胆汁淤积症)。19例为特发性婴儿胆汁淤积症。3例有其他因素,但他们都患有川崎病。71例诊断不明确。A 组和 B 组在性别和年龄方面没有统计学差异(P>0.05)。A组的碱性磷酸酶(ALP)和胆汁酸水平明显高于B组,PPχ2=3.89,PPC结论:婴儿胆汁淤积症的病因多种多样。ALP、胆汁酸、GGT、DBil和白蛋白水平可作为早期鉴别遗传性代谢性肝病和胆道闭锁的简单指标。在排除胆道闭锁后,应通过积极完成遗传代谢基因检测,尽早确定胆汁淤积症的病因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
[Analysis of the etiology and clinical indicators of infantile cholestasis].

Objective: To explore the disease spectrum and corresponding clinical indicators of infantile cholestasis so as to provide a basis for the diagnosis of this type of disease at an early stage. Methods: The clinical data was collected from 203 hospitalized children diagnosed with infantile cholestasis at the Department of Gastroenterology of Maternal and Child Health Care, Guiyang City, from January 2018 to March 2023, including 130 males and 73 females. Patients general condition, personal history, and blood biochemical test indicators, including liver and coagulation function, blood ammonia, blood lipid profile, blood sugar, TORCH, thyroid function, and others, were retrospectively analyzed after admission. Cholangiography and high-throughput gene sequencing were performed in certain patients. The etiology of the enrolled cases were analyzed. Children's clinical data were compared with distinct inherited metabolic liver diseases (Group A) and biliary atresia (Group B). The statistical analysis was conducted using the t-test, Mann-Whitney test, Kruskal-Wallis test, or χ2 test, according to different data. Results: In 33 cases, infectious factors-primarily CMV infection-were the etiology of cholestasis. Forty cases had aberrant bile duct development, primarily biliary atresia, choledochal cysts, and intrahepatic bile duct dysplasia. In 26 cases, genetic metabolic factors mainly included citrin protein deficiency, sodium-taurocholate co-transporting polypeptide deficiency, and Alagille syndrome. 11 cases had drug/poisoning factors (parenteral nutrition-associated cholestasis). 19 cases had idiopathic infantile cholestasis. Three cases had other factors; however, all of them had Kawasaki disease. 71 cases had an unclear diagnosis. There was no statistically significant difference in terms of gender and age between groups A and B (P>0.05). The alkaline phosphatase (ALP) and bile acid levels were significantly higher in Group A than Group B, with a P<0.05, while the gamma glutamyltransferase (GGT), direct bilirubin (DBil), and albumin levels were lower than those in Group B, with a P<0.05. The cytomegalovirus infection rate was higher in Group B (62.50%) than Group A (34.62%), and the difference between the two groups was statistically significant (χ2=3.89, P<0.05). The alanine aminotransferase, aspartate aminotransferase, GGT, DBil, and albumin were significantly lower in patients with citrin protein deficiency than those in patients with biliary atresia, while ALP, bile acid, and blood ammonia were higher than those in patients with biliary atresia. Patients with sodium-taurocholate co-transporting polypeptide deficiency had higher bile acid than patients with biliary atresia, while the DBil was lower than that in patients with biliary atresia, and the difference was statistically significant (P<0.05). Conclusion: Infantile cholestasis etiology is diverse. ALP, bile acids, GGT, DBil, and albumin levels can serve as simple indicators for early-stage differentiation between inherited metabolic liver disease and biliary atresia. The cholestasis etiology should be determined as early as possible following biliary atresia exclusion by actively completing genetic metabolic gene detection.

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中华肝脏病杂志
中华肝脏病杂志 Medicine-Medicine (all)
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1.20
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7574
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