Viemann M, Peter M, López-Siguero J P, Simic-Schleicher G, Sippell W G
Division of Pediatric Endocrinology, Department of Pediatrics, Christian Albrechts University of Kiel, Germany.
J Clin Endocrinol Metab. 2001 May;86(5):2056-9. doi: 10.1210/jcem.86.5.7449.
Pseudohypoaldosteronism type 1 (PHA1) is characterized by neonatal salt wasting resistant to mineralocorticoids. There are 2 forms of PHA1: the autosomal recessive form with symptoms persisting into adulthood, caused by mutations in the amiloride-sensitive luminal sodium channel, and the autosomal dominant or sporadic form, which shows milder symptoms that remit with age. Mutations in the gene encoding the human mineralocorticoid receptor (hMR) are, at least in some patients, responsible for the latter form of PHA1. We here report the results of a genetic study in a sporadic case and in 5 affected patients from 2 families with autosomal dominant PHA1. In the sporadic case we identified a new frameshift mutation, Ins2871C, in exon 9 of the hMR gene. Family members were asymptomatic and had no mutation. This mutation is the first described in exon 9 and impairs the last 27 amino acids of the hormone-binding domain. In 2 kindreds with autosomal dominant PHA1 we found no mutation of the hMR gene. Our results confirm the hypothesis that autosomal dominant or sporadic PHA1 is a genetically heterogeneous disease involving other, as yet unidentified, genes.
1型假性醛固酮减少症(PHA1)的特征是新生儿盐耗,对盐皮质激素有抵抗。PHA1有两种形式:常染色体隐性形式,症状持续至成年,由阿米洛利敏感的管腔钠通道突变引起;常染色体显性或散发形式,症状较轻,随年龄缓解。至少在一些患者中,编码人类盐皮质激素受体(hMR)的基因突变是导致后一种形式PHA1的原因。我们在此报告了对一例散发病例以及来自两个常染色体显性PHA1家族的5名患病患者进行基因研究的结果。在散发病例中,我们在hMR基因的外显子9中鉴定出一个新的移码突变Ins2871C。家族成员无症状且无突变。该突变是首次在外显子9中被描述,它损害了激素结合域的最后27个氨基酸。在两个常染色体显性PHA1家族中,我们未发现hMR基因的突变。我们的结果证实了以下假设:常染色体显性或散发的PHA1是一种基因异质性疾病,涉及其他尚未确定的基因。
