Hydrochlorothiazide with salt restriction in nonsurgical hypoparathyroidism: a placebo-controlled single-blinded randomized crossover trial assessing efficacy and safety

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Dades bibliogràfiques
Publicat a:	JBMR Plus vol. 9, no. 12 (Dec 2025)
Autor principal:	Jha, Vivek
Altres autors:	Mukherjee, Soham, Bhadada, Sanjay Kumar, Sahni, Nancy, Ram, Sant, Dutta, Pinaki
Publicat:	Oxford University Press
Matèries:	Clinical trials Nutrient deficiency Bone turnover Parathyroid hormone Sodium Collagen Placebos Sensitivity analysis Renal function Calciuria Hydrochlorothiazide Hypokalemia Calcium carbonate Excretion Homeostasis Statistical analysis Calcium (blood) Hypoparathyroidism Calcium (urinary) Body weight Calcium homeostasis Calcitriol
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Resum:	In this single-center, randomized, placebo-controlled, single-blinded, crossover trial (Clinical Trial Registry-India: CTRI/2024/08/090041), we evaluated the efficacy and safety of low-dose hydrochlorothiazide (HCTZ) in adults with nonsurgical hypoparathyroidism (excluding autoimmune and obvious syndromic forms). After stabilization on fixed doses of calcium carbonate and calcitriol under a controlled low-sodium diet, 26 participants received HCTZ (12.5-25 mg/d) or placebo for 7 d, with a 15-d washout before crossover, followed by an optional 4-wk open-label HCTZ extension. The primary outcome was change in serum calcium; secondary outcomes included change in 24-h urinary calcium (UCa), fractional calcium excretion, urinary sodium, and bone turnover markers (β-CTX and P1NP). Compared to baseline (8.61 ± 0.32 mg/dL), serum calcium increased significantly with HCTZ at day 5 (9.01 ± 0.46 mg/dL) and day 8 (9.04 ± 0.52 mg/dL; p < .001), while no significant change occurred with placebo. Hydrochlorothiazide reduced 24-h UCa by −26.3% at day 8 (vs +4.7% with placebo; p < .001). These effects remained robust in sensitivity analyses adjusting for urinary sodium and when expressed per kg body weight. Fractional calcium excretion fell by 29.9% with HCTZ (p < .001). A small but statistically significant decline in serum potassium was observed at day 8 (from 4.18 to 3.95 mEq/L; p < .001), though values remained within the normal range, no participants developed hypokalemia; renal function and intact PTH (iPTH) were stable. During the extension phase, serum calcium levels rose while UCa excretion declined significantly, without any reported adverse effects. These findings indicate that low-dose HCTZ with sodium restriction safely improves calcium homeostasis in nonsurgical hypoparathyroidism—raising serum calcium and reducing calciuria—with good tolerability. Hydrochlorothiazide offers a cost-effective adjunct to standard therapy and warrants further investigation for long-term outcomes.Lay Summary In 26 adults with nonsurgical hypoparathyroidism, low-dose hydrochlorothiazide (12.5-25 mg daily) raised serum calcium levels and reduced calcium loss in urine within 1 wk, without causing harmful side effects. A 4-wk extension confirmed sustained benefits. This simple, safe, and affordable treatment may improve calcium control alongside standard therapy and may reduce kidney-related complications.
ISSN:	2473-4039
DOI:	10.1093/jbmrpl/ziaf174
Font:	Health & Medical Collection