Cho Hee-Won, Lee Sang Taek, Cho Heeyeon, Cheong Hae Il
Department of Pediatrics, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea.
Department of Pediatrics, Seoul National University Children's Hospital, Seoul, Korea.
Korean J Pediatr. 2016 Nov;59(Suppl 1):S103-S106. doi: 10.3345/kjp.2016.59.11.S103. Epub 2016 Nov 30.
Bartter syndrome (BS) is an inherited renal tubular disorder characterized by low or normal blood pressure, hypokalemic metabolic alkalosis, and hyperreninemic hyperaldosteronism. Type III BS is caused by loss-of-function mutations in encoding basolateral ClC-Kb. The clinical phenotype of patients with mutations has been known to be highly variable, and cases that are difficult to categorize as type III BS or other hereditary tubulopathies, such as Gitelman syndrome, have been rarely reported. We report a case of a 10-year-old Korean boy with atypical clinical findings caused by a novel mutation. The boy showed intermittent muscle cramps with laboratory findings of hypokalemia, severe hypomagnesemia, and nephrocalcinosis. These findings were not fully compatible with those observed in cases of BS or Gitelman syndrome. The mutation analysis revealed a heterozygous c.139G>A transition in exon 13 [p.Gly(GGG)465Glu(GAG)]. This change is not a known mutation; however, the clinical findings and in silico prediction results indicated that it is the underlying cause of his presentation.
巴特综合征(BS)是一种遗传性肾小管疾病,其特征为血压低或正常、低钾性代谢性碱中毒以及高肾素性醛固酮增多症。III型巴特综合征由编码基底外侧ClC-Kb的功能丧失性突变引起。已知具有该突变的患者临床表型高度可变,而难以归类为III型巴特综合征或其他遗传性肾小管病(如吉特林综合征)的病例鲜有报道。我们报告一例10岁韩国男孩,因一种新的突变导致非典型临床表现。该男孩表现为间歇性肌肉痉挛,实验室检查发现低钾血症、严重低镁血症和肾钙质沉着症。这些发现与巴特综合征或吉特林综合征病例中观察到的情况不完全相符。突变分析显示外显子13存在杂合性c.139G>A转换[p.甘氨酸(GGG)465谷氨酸(GAG)]。这一变化并非已知突变;然而,临床发现和计算机模拟预测结果表明,它是该男孩临床表现的潜在病因。
