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Gitelman syndrome combined with growth hormone deficiency: Three cases report

机译:Gitelman综合征联合生长激素缺乏:三种案例报告

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Rationale: Gitelman syndrome (GS) is a rare autosomal recessive hereditary salt-losing tubulopathy caused by loss-of-function mutations in the SLC12A3 gene. It is usually characterized by hypokalemia, metabolic alkalosis, hypomagnesemia, and hypocalciuria. There are only a few reports on GS combined with growth hormone deficiency (GHD). Patient concerns: Three patients presented with weakness, spasm, and growth retardation, respectively. Diagnoses: GS was diagnosed based on the clinical symptoms, laboratory test results, and genetic analysis . GH stimulation tests were performed when the magnesium level returned to normal under magnesium oxide (MgO) therapy . Interventions: Initially, all patients received oral replacement of MgO and potassium chloride, and 2 of them received simultaneous spironolactone therapy . Recombinant human growth hormone (rhGH) therapy was initiated after they were diagnosed with GHD. Outcomes: All 3 patients exhibited satisfactory growth velocity and normal serum magnesium level, although the potassium level was still slightly lower than normal. Lessons: We suggest that all GS patients should undergo genetic evaluation, especially regarding SLC12A3 gene mutation. GHD should be considered if these patients have short stature. rhGH therapy is useful for stimulating the patients’ growth, and it may increase the serum magnesium level.
机译:理由:Gitelman综合征(GS)是由SLC12A3基因中的功能突变损失引起的稀有常血糖隐性遗传遗传失调的微生物病变。它的特征在于低钾血症,代谢碱中毒,低钙血症和低钙尿。 GS只有少数报告结合生长激素缺乏(GHD)。患者涉及:三名患者分别呈现弱点,痉挛和生长延迟。诊断:基于临床症状,实验室测试结果和遗传分析诊断出GS。当氧化镁(MgO)治疗下镁水平恢复到正常时,进行GH刺激测试。干预措施:最初,所有患者均接受口服替代MgO和氯化钾,其中2个接受了同时螺旋烯酮治疗。在诊断患有GHD后,启动重组人生长激素(RHGH)治疗。结果:所有3例患者表现出令人满意的生长速度和正常的血清镁水平,尽管钾水平仍然略低于正常。课程:我们建议所有GS患者应接受遗传评估,特别是关于SLC12A3基因突变。如果这些患者身材矮小,应考虑GHD。 RHGH治疗可用于刺激患者的生长,并且可能会增加血清镁水平。

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