Department of Pediatrics, Obihiro Kyoukai Hospital, Obihiro 080-0805, Japan.
Endocr J. 2013;60(1):51-5. doi: 10.1507/endocrj.ej12-0248. Epub 2012 Oct 28.
Isolated hypoaldosteronism is a rare and occasionally life-threatening cause of salt wasting in infancy. A 2-month-old Japanese boy of unrelated parents was examined for failure to thrive and poor weight gain. Laboratory findings were hyponatremia, hyperkalemia, high plasma renin and low aldosterone levels. Spot urine analysis by gas chromatography-mass spectrometry (GC-MS) showed that urinary excretion of corticosterone metabolites was elevated. Whereas excretion of 18-hydroxycortricosterone metabolites was within the normal range, excretion of aldosterone metabolites was undetectable. The patient was therefore suspected to have aldosterone synthase deficiency type 1. Sequence analysis of CYP11B2, the gene encoding aldosterone synthase (CYP11B2), showed that the patient was a compound heterozygote for c.168G>A, p.W56X in exon 1 and c.1149C>T, p.R384X in exon 7. p.W56X was inherited from his mother and p.R384X was from his father. Since both alleles contain nonsense mutations, a lack of CYP11B2 activity was speculated to cause his condition. To our knowledge, this is the first Japanese patient in which the molecular basis of aldosterone synthase deficiency type 1 has been clarified. This case also indicates that spot urinary steroid analysis is useful for diagnosis.
孤立性醛固酮缺乏症是婴儿期盐耗性疾病的罕见病因,偶尔会危及生命。一名 2 月龄、非近亲父母所生的日本男婴因生长发育迟缓且体重增加不良而就诊。实验室检查发现低钠血症、高钾血症、血浆肾素升高和醛固酮水平降低。气相色谱-质谱联用(GC-MS)检测尿液提示皮质酮代谢物排泄增加。18-羟皮质酮代谢物排泄正常,但醛固酮代谢物检测不到。因此,该患者疑诊为醛固酮合酶缺乏症 1 型。CYP11B2 基因(编码醛固酮合酶)的序列分析显示,患者为 CYP11B2 外显子 1 的 c.168G>A、p.W56X 和外显子 7 的 c.1149C>T、p.R384X 复合杂合突变。p.W56X 遗传自母亲,p.R384X 遗传自父亲。由于两个等位基因均包含无义突变,推测 CYP11B2 缺乏导致了该患者的疾病。据我们所知,这是首例阐明醛固酮合酶缺乏症 1 型分子基础的日本患者。该病例还表明,尿液类固醇分析有助于诊断。
