Lin Shih-Hua, Shiang Jen-Chuan, Huang Che-Chung, Yang Sung-Sen, Hsu Yu-Juei, Cheng Chih-Jen
Division of Nephrology, Department of Medicine, Tri-Service General Hospital, Number 325, Section 2, Cheng-Kung Road, Neihu 114, Taipei, Taiwan.
J Clin Endocrinol Metab. 2005 May;90(5):2500-7. doi: 10.1210/jc.2004-1905. Epub 2005 Feb 1.
Inactivation mutations of the luminal thiazide-sensitive NaCl cotransporter (NCC) in the distal convoluted tubules or the basolateral chloride channel (CLCNKB) in the distal nephron are the most common genetic mutations in Gitelman's syndrome (GS) or Bartter's syndrome (BS). We conducted clinical and molecular studies in Chinese patients with GS or BS. Twenty patients with chronic hypokalemia (15 males and five females, age 25 +/- 7 yr) from 15 unrelated Chinese families were investigated. All had renal K+ wasting, metabolic alkalosis, and normotension. The urinary calcium excretion rate was used to distinguish between BS or GS on clinical grounds. Clinical symptoms and biochemical studies were recorded. Molecular analysis included PCR single-strand confirmational polymorphism, direct sequencing of both the NCC and CLCNKB genes, and restriction fragment length polymorphism. Sixteen patients had a clinical diagnosis of GS with hypocalciuria and four BS without hypocalciuria. Four of these 20 patients did not have hypomagnesemia. The males had severe hypokalemia [1.9 +/- 0.4 mEq/liter (mmol/liter)] with paralytic episodes, whereas females had moderate hypokalemia [2.6 +/- 0.2 mEq/liter (mmol/liter)] and less severe symptoms. There were no mutations detected in CLCNKB. Twelve NCC mutations, including six novel mutations and nine recurrent ones, were identified. Allele frequency of the detected NCC mutations was 3% in 100 healthy subjects. Some GS patients with NCC mutations may have normocalciuria and/or normomagnesemia. Gender differences may account for phenotype variability. Screening of these identified NCC mutations remains the gold standard for the diagnosis of GS.
远曲小管腔面噻嗪类敏感型氯化钠协同转运蛋白(NCC)或远端肾单位基底外侧氯通道(CLCNKB)的失活突变是吉特曼综合征(GS)或巴特综合征(BS)中最常见的基因突变。我们对中国的GS或BS患者进行了临床和分子研究。对来自15个无亲缘关系的中国家庭的20例慢性低钾血症患者(15例男性和5例女性,年龄25±7岁)进行了调查。所有患者均有肾钾流失、代谢性碱中毒和血压正常。尿钙排泄率用于临床区分BS或GS。记录临床症状和生化研究结果。分子分析包括聚合酶链反应单链构象多态性、NCC和CLCNKB基因的直接测序以及限制性片段长度多态性。16例患者临床诊断为伴有低钙尿症的GS,4例为不伴有低钙尿症的BS。这20例患者中有4例没有低镁血症。男性有严重低钾血症[1.9±0.4毫当量/升(毫摩尔/升)]并伴有麻痹发作,而女性有中度低钾血症[2.6±0.2毫当量/升(毫摩尔/升)]且症状较轻。未在CLCNKB中检测到突变。共鉴定出12个NCC突变,包括6个新突变和9个重复突变。在100名健康受试者中,检测到的NCC突变的等位基因频率为3%。一些具有NCC突变的GS患者可能有正常钙尿症和/或正常镁血症。性别差异可能解释表型变异性。对这些已鉴定的NCC突变进行筛查仍然是诊断GS的金标准。
