1例父源性3-甲基巴豆酰辅酶A羧化酶缺乏症的临床特点及家系分析  

作　　者：陈燕茹 苏雅君 林壹明 林卫华 CHEN Yan-ru;SU Ya-jun;LIN Yi-ming;LIN Wei-hua(The Graduate School of Fujian Medical University,Fuzhou 350000,Fujian,China;Neonatal Disease Screening Center,Quanzhou Maternity and Children's Hospital,Quanzhou 362000,Fujian,China;Department of Child Healthcare,Quanzhou Maternity and Children's Hospital,Quanzhou 362000,Fujian,China;The School of Clinical Medicine,Fujian Medical University,Fuzhou 350000,Fujian,China)

机构地区：[1]福建医科大学研究生院,福建福州350000 [2]泉州市妇幼保健院·儿童医院新生儿疾病筛查中心,福建泉州362000 [3]泉州市妇幼保健院·儿童医院儿童保健科,福建泉州362000 [4]福建医科大学临床医学部,福建福州350000

出　　处：《罕少疾病杂志》2024年第6期4-7,共4页Journal of Rare and Uncommon Diseases

基　　金：泉州市科技计划资助基金项目(Grant No.2021C055R)。

摘　　要：目的报道1例新生儿疾病筛查发现父源性3-甲基巴豆酰辅酶A羧化酶缺乏症(3-Methylcrotonyl-CoA carboxylase deficiency,MCCD)的临床特点、基因诊断及家系分析。方法回顾性分析1例新生儿疾病筛查发现3-羟基异戊酰肉碱(3-hydroxyisovalerylcarnitine,C5OH)增高的新生儿,尿有机酸分析及基因检测证实为父源性MCCD。结果该新生儿初筛血串联质谱C5OH轻度增高,尿有机酸结果正常,其父亲血串联质谱示C5OH明显增高,血浆游离肉碱降低,母亲血串联质谱正常。基因分析结果证实新生儿为MCCC1基因c.980C>G(p.Ser327Ter)杂合变异,其父亲为MCCC1基因c.980C>G(p.Ser327Ter)纯合无义变异。结论新生儿筛查发现持续轻度C5OH水平升高的情况时应考虑父源性MCCD。定期随访仍然是MCCD治疗管理的重心。Objective To report the clinical characteristics,gene diagnosis and family analysis of a case of paternal 3-methylcrotonyl-CoA carboxylase deficiency(MCCD)found in Newborn screening(NBS).MethodsRetrospective analysis was performed on a newborn who was found to have increased 3-hydroxyisovaleryl carnitine(C5OH)through NBS.Urine organic acid analysis(GC/MS)was carried out on him.His parents performed tandem mass spectrometry(MS/MS).Finally,the clinical diagnosis was confirmed by gene detection.ResultsSlight elevated plasma C5OH concentration was detected via MS/MS by NBS in the newborn,whose urine GC/MS was normal.Evaluation of his parents revealed increased C5OHand low C0 in his father,while normal MS/MS results were achieved from his mother.Sequencing analyses demonstrated that the newborn carries a single mutant methylcrotonyl-CoA carboxylase subunit 1(MCCC1)nonsense allele(c.980C>G)and a homozygous nonsense variation c.980C>G was found in his father.Conclusions Paternal MCCD should be considered in neonates exhibiting a persistent slight increase in C5OH levels.Basic follow-up treatments remain the cornerstone of successfully mitigating the lifelong effects of MCCD.

关 键 词：父源性3-甲基巴豆酰辅酶A羧化酶缺乏症 3-羟基异戊基肉碱 新生儿疾病筛查 MCCC1基因 

分 类 号：R725.8[医药卫生—儿科]