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Case Report: Gitelman or Bartter type 3 syndrome? A case of distal convoluted tubulopathy caused by CLCNKB gene mutation

机译:病例报告:吉特曼还是巴特3型综合征?由CLCNKB基因突变引起的远曲性肾小管病变一例

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摘要

A 32-year-old woman with no significant medical history was sent to our consultation due to hypokalaemia (<3.0 mmol/l). Her main complaints were longstanding polyuria and nocturia. Physical examination was normal. Basic investigations showed normal renal function, low serum potassium (2.7 mmol/l) and magnesium (0.79 mmol/l), metabolic alkalosis (pH 7.54; bicarbonate 32.5 mmol/l), elevated urinary potassium (185 mmol/24 h) and normal urinary calcium (246 mg/24 h). Thiazide test revealed blunted response. Chronic vomiting and the abuse of diuretics were excluded. Genetic tests for SLC12A3 gene mutation described in Gitelman syndrome (GS) came negative. CLCNKB gene mutation analysis present in both GS and Bartter (BS) type 3 syndromes was positive. The patient is now being treated with potassium and magnesium oral supplements, ramipril and spironolactone with stable near-normal potassium and magnesium levels. This article presents the case of a patient with hypokalaemia caused by CLCNKB gene mutation hard to categorise as GS or BS type 3.
机译:由于低钾血症(<3.0 mmol / l),一名没有明显病史的32岁妇女被送往我们的咨询。她的主要主诉是长期以来的多尿症和夜尿症。体检正常。基本检查显示肾功能正常,血清钾(2.7 mmol / l)和镁(0.79 mmol / l)低,代谢性碱中毒(pH 7.54;碳酸氢盐32.5 mmol / l),尿钾升高(185 mmol / 24 h)和正常尿钙(246 mg / 24 h)。噻嗪试验显示反应迟钝。排除了慢性呕吐和利尿剂滥用。 Gitelman综合征(GS)中描述的SLC12A3基因突变的遗传测试呈阴性。 GS和Bartter(BS)3型综合征中均存在的CLCNKB基因突变分析为阳性。该患者正在接受钾和镁口服补充剂,雷米普利和螺内酯,其钾和镁水平稳定在接近正常水平。本文介绍了由CLCNKB基因突变引起的低钾血症患者的案例,这种突变很难归类为GS或BS 3型。

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