临床儿科杂志 ›› 2023, Vol. 41 ›› Issue (4): 259-265.doi: 10.12372/jcp.2023.22e1714

• 新生儿疾病专栏 • 上一篇    下一篇

尿素循环障碍所致新生儿高氨血症基因筛查和早期干预

张银纯1, 莫文辉2, 白波3, 陈进勉4, 石聪聪5, 古霞1,5, 肖昕1,5(), 郝虎1,5()   

  1. 1.中山大学附属第六医院儿科(广东广州 510655)
    2.佛山复星禅诚医院(广东佛山 528000)
    3.南方医科大学附属花都医院/广州市花都区人民医院新生儿科(广东广州 510800)
    4.湛江市妇幼保健计划生育服务中心(广东湛江 524000)
    5.中山大学附属第六医院遗传代谢病实验室(广东广州 510655)
  • 收稿日期:2023-01-04 出版日期:2023-04-15 发布日期:2023-04-07
  • 通讯作者: 肖昕,郝虎 E-mail:haohu@mail.sysu.edu.cn;xiaoxin2@mail.sysu.edu.cn

Genetic screening and early intervention in neonatal hyperammonemia caused by urea cycle disorder

ZHANG Yinchun1, MO Wenhui2, BAI Bo3, CHEN Jinmian4, SHI Congcong5, GU Xia1,5, XIAO Xin1,5(), HAO Hu1,5()   

  1. 1. Department of Pediatrics, The Sixth Affiliated Hospital, Sun Yat-Sen University, Guangzhou 510655, Guangdong, China
    2. Foshan Fosun Chancheng Hospital, Foshan 528000, Guangdong, China
    3. Department of Neonatology, Huadu Hospital Affiliated to Southern Medical University, Huadu District People's Hospital, Guangzhou 510800, Guangdong, China
    4. Zhanjiang Maternal and Child Health and Family Planning Service Center, Zhanjiang 524000, Guangdong, China
    5. Inborn Errors of Metabolism Laboratory, The Sixth Affiliated Hospital, Sun Yat-Sen University, Guangzhou 510655, Guangdong, China
  • Received:2023-01-04 Online:2023-04-15 Published:2023-04-07
  • Contact: XIAO Xin,HAO Hu E-mail:haohu@mail.sysu.edu.cn;xiaoxin2@mail.sysu.edu.cn

摘要:

目的 探讨广东地区新生儿尿素循环障碍(UCD)的发病率,以实现UCD相关新生儿高氨血症(NHA)早期识别与干预。方法 收集2019年至2022年广东地区多中心38 159个新生儿基因筛查数据,统计UCD新生儿基因阳性率,分析基因筛查中确诊的9例与UCD相关NHA患儿临床干预和疗效。 结果 UCD基因阳性率0.472%,Citrin缺陷病最常见(基因阳性率0.314%)。其中3例Citrin缺陷病均为SLC25A13基因c.852_855delTATG纯合致病性变异,不同的确诊和临床干预时期,预后不同。另外6例UCD相关NHA患儿起病早,病情进展快,经积极早期对症治疗后,2例瓜氨酸血症I型患儿好转,4例患儿死亡和1例失访。 结论 NHA的病因复杂多样,以UCD最为常见,临床表现缺乏特异性,容易漏诊、误诊,早期血、尿代谢筛查联合UCD相关基因筛查可实现UCD相关NHA的早期识别和诊疗,可指导遗传咨询和再次妊娠的产前诊断。

关键词: 高氨血症, 遗传代谢病, 尿素循环障碍, 早期诊疗, 新生儿

Abstract:

Objective To explore the prevalence of neonatal urea circulation disorder (UCD) by genetic screening and achieve the early identification and intervention of neonatal hyperammonemia (NHA) caused by UCD in Guangdong province. Methods The gene screening data of 38159 neonates from multiple centers in Guangdong region from 2019 to 2022 were collected, and the gene positive rate of UCD neonates was calculated. Meanwhile, the clinical intervention and efficacy of 9 children with UCD related NHA were further analyzed. Results The gene positive rate of UCD in newborns in Guangdong was 0.472%, and citrin deficiency was the commonest (0.314%). All three cases of citrin deficiency had homozygous variation of c.852_855delTATG in SLC25A13 gene. Due to the different diagnosis time and clinical intervention period, the prognosis of children is also different. Six children with UCD related NHA had early onset and advanced progression. After active early symptomatic treatment, two patients with citrullinemia typeⅠimproved, four patients died and one was lost to follow-up. Conclusions The etiology of NHA is complex and diverse, and UCD is the commonest. Its clinical manifestations lack specificity, and it is easy to be missed and misdiagnosed. Early blood and urine metabolism screening combined with UCD-related gene screening can achieve early identification, diagnosis and treatment of UCD-related NHA, and can guide genetic counseling and prenatal diagnosis of another pregnancy.

Key words: hyperammonemia, genetic metabolic disease, urea circulation disorder, early diagnosis and treatment, neonatal