摘要
目的分析4个甲基丙二酸尿症(MMA)的家系基因突变情况,阐明开展MMA基因突变分析及产前诊断的意义。方法对诊断为MMA的先证者或其父母行相关基因的高通量测序,确定基因突变位点,并采用聚合酶链反应和直接测序法对家系行一代测序验证。家系1、3、4于先证者母亲再次妊娠11~13周时超声引导下行绒毛活检,进行早期产前诊断。结果家系1先证者父亲检出MUT基因c.656A〉T杂合突变,先证者母亲检出c.729-730ins TT杂合突变;早期产前诊断发现胎儿为c.656A〉T和c.729-730ins TT双重杂合突变,终止妊娠。家系2先证者检出MUT基因c.1106G〉A和c.755-756ins A双重杂合突变,c.1106G〉A来自父亲,c.755-756ins A来自母亲。家系3先证者检出MMACHC基因c.217C〉T和c.609G〉A双重杂合突变,c.217C〉T来自父亲,c.609G〉A来自母亲;产前诊断提示胎儿携带c.609G〉A杂合突变,胎儿出生时脐血检测结果与产前诊断一致。家系4先证者检出MMACHC基因c.609G〉A和c.567dup T双重杂合突变,c.609G〉A来自父亲,c.567dup T来自母亲;产前诊断提示胎儿携带c.567dup T杂合突变,胎儿顺利出生,脐血检测结果与产前诊断一致。结论明确基因突变有助于MMA家系行产前诊断,避免缺陷患儿出生。
ObjectiveTo study gene mutations in four pedigrees with methymalonic aciduria, as well as the feasibility of prenatal diagnosis of methymalonic aciduria.MethodsHigh-throughput sequencing was performed for related genes in the peripheral blood of children or parents who were diagnosed with methymalonic aciduria to identify the loci with mutations. Then ampliifcation primers were designed for each locus, and PCR and direct sequencing were performed to validate the sequencing in the ifrst generation in the four pedigrees. Whether the mutations were pathogenic were determined with reference to literature review and medical history. In the pedigrees 1, 3, and 4, ultrasound-guided chorionic villi biopsy was performed at weeks 11-13 of pregnancy to perform early prenatal diagnosis.ResultsIn pedigree 1, c.656A〉T and c.729-730insTT heterozygous mutations in the MUT gene were detected in the proband’s father and mother, respectively. Early prenatal diagnosis showed c.656A〉T and c.729-730insTT double heterozygous mutations in the fetus. The couple decided to terminate pregnancy. In pedigree 2, c.1106G〉A and c.755-756insA double heterozygous mutations in the MUT gene were detected in the proband. c.1106G〉A came from the father and c.755-756insA came from the mother. In pedigree 3, c.217C〉T and c.609G〉A double heterozygous mutations in the MMACHC gene were detected in the proband. c.217C〉T came from the father and c.609G〉A came from the mother. Prenatal diagnosis showed c.609G〉A heterozygous mutation in the fetus. The baby was successfully delivered, and the result of umbilical cord blood testing was consistent with the prenatal diagnosis. In pedigree 4, c.609G〉A and c.567dupT double heterozygous mutations in the MMACHC gene were detected in the proband. c.609G〉A came from the father 〈br〉 and c.567dupT came from the mother. Prenatal diagnosis showed c.567dupT heterozygous mutation in the fetus. The baby was successfully delivered, and the result of umbilical cord blood testing was consistent with the prenatal diagnosis. ConclusionsIdentiifcation of gene mutations helps with prenatal diagnosis in pedigrees with methymalonic aciduria.
出处
《中国当代儿科杂志》
CAS
CSCD
北大核心
2016年第10期1013-1018,共6页
Chinese Journal of Contemporary Pediatrics
关键词
甲基丙二酸尿症
基因突变
产前诊断
家系研究
Methymalonic aciduria
Gene mutation
Prenatal diagnosis
pedigree study