Reiss J, Christensen E, Dorche C
Institut für Humangenetik der Universität, Göttingen, Germany.
Prenat Diagn. 1999 Apr;19(4):386-8. doi: 10.1002/(sici)1097-0223(199904)19:4<386::aid-pd550>3.0.co;2-#.
Molybdenum cofactor (MoCo) deficiency leads to a combined deficiency of the molybdo-enzymes sulphite oxidase, xanthine dehydrogenase and aldehyde oxidase. No therapy is known for this rare disease, which results in neonatal seizures and other neurological symptoms identical to sulphite oxidase deficiency. It is inherited autosomal-recessively and leads to early childhood death. Prenatal diagnosis has been performed since 1983 by the measurement of sulphite oxidase activity, but no enzymatic carrier diagnosis is possible. The human genes necessary for MoCo biosynthesis have recently been cloned and mutations in the bicistronic MOCS1 gene could be identified in most European patients. In a Danish family we have now performed enzymatic and molecular genetic analysis in parallel after chorionic villus sampling. The sulphite oxidase activity in uncultured CVS material was found to be normal. A MOCS1 splice site mutation, found homozygous in the affected patient, was found in a heterozygous state in cultured chorionic cells. This confirmed that the fetus was not affected, since heterozygous carriers of a MoCo deficiency allele do not display any symptoms.
钼辅因子(MoCo)缺乏会导致亚硫酸盐氧化酶、黄嘌呤脱氢酶和醛氧化酶这几种含钼酶的联合缺乏。这种罕见疾病尚无已知疗法,会导致新生儿惊厥以及与亚硫酸盐氧化酶缺乏相同的其他神经症状。它以常染色体隐性方式遗传,会导致幼儿期死亡。自1983年以来,通过测量亚硫酸盐氧化酶活性进行产前诊断,但无法进行酶学携带者诊断。最近已克隆出MoCo生物合成所需的人类基因,并且在大多数欧洲患者中可鉴定出双顺反子MOCS1基因中的突变。在一个丹麦家庭中,我们现在在绒毛取样后并行进行了酶学和分子遗传学分析。未培养的绒毛取样组织中的亚硫酸盐氧化酶活性被发现正常。在受影响患者中发现纯合的一个MOCS1剪接位点突变,在培养的绒毛细胞中呈杂合状态被发现。这证实胎儿未受影响,因为MoCo缺乏等位基因的杂合携带者不表现出任何症状。
