Baldinger S, Pierpont M E, Wenger D A
Clin Genet. 1987 Feb;31(2):70-6. doi: 10.1111/j.1399-0004.1987.tb02772.x.
Arylsulfatase A (ASA) deficiency is the cause of early and late onset metachromatic leukodystrophy (MLD). Low ASA levels are detected in some healthy individuals who are pseudodeficient (PD). PD individuals can be distinguished, because PD fibroblasts hydrolyze 14C-sulfatide at similar rates to normal fibroblasts. This has also been demonstrated in amniocytes and chorionic villi (CV). The genetic basis for PD is not clearly understood and is most likely heterogeneous with respect to allelic mutations of the ASA gene. It is hypothesized that the PD phenotype can either be due to PD/PD or PD/MLD genotypes, only the latter representing a potential risk to offspring. We report an unusual family where two siblings, both carriers of the classic late infantile MLD allele, are married to unrelated PD individuals. One couple has two PD offspring; their "at risk" status, due to the lack of an affected offspring is in question. The other couple terminated a fetus determined to be affected with a "MLD variant", most likely a compound heterozygote. Cautions prenatal counseling of PD families is essential. The population frequency of the PD phenotype is unknown.
芳基硫酸酯酶A(ASA)缺乏是早发型和晚发型异染性脑白质营养不良(MLD)的病因。在一些假性缺乏(PD)的健康个体中检测到低ASA水平。可以区分出PD个体,因为PD成纤维细胞水解14C - 硫脂的速率与正常成纤维细胞相似。这在羊水细胞和绒毛膜绒毛(CV)中也得到了证实。PD的遗传基础尚不清楚,很可能在ASA基因的等位基因突变方面具有异质性。据推测,PD表型可能是由于PD/PD或PD/MLD基因型,只有后者对后代构成潜在风险。我们报告了一个不同寻常的家庭,其中两个携带经典晚发性婴儿型MLD等位基因的兄弟姐妹与不相关的PD个体结婚。一对夫妇有两个PD后代;由于没有患病后代,他们的“风险”状况存疑。另一对夫妇终止了一个被确定患有“MLD变异型”的胎儿,很可能是复合杂合子。对PD家庭进行谨慎的产前咨询至关重要。PD表型的人群频率尚不清楚。
