Treatment of neurohypophyseal diabetes insipidus

Abstract

Context: In recent years, there have been several improvements in the treatment of neurohy-pophyseal diabetes insipidus (DI). They include new formulations of the vasopressin analog, des-mopressin; a better understanding of the effect of fluid intake on dosing; and more information about treatments of infants, children, and pregnant women who present special challenges. This review aims to summarize past and current information relative to the safety and efficacy of treatments for the types of DI caused by a primary deficiency of vasopressin. Evidence Acquisition: The review is based on publications identified primarily by a PubMed search of the international literature without limitations of date. Evidence Synthesis: In acute settings where fluid intake is determined by factors other than thirst, desmopressin should be given iv in doses that have a short duration of action and can be adjusted quickly in accordance with changes in hydration as indicated by plasma sodium. In ambulatory patients, the oral formulations (tablet or melt) are preferred for their convenience. If fluid intake is regulated normally by the thirst mechanism, the tablets or melt can be taken safely 1 to 3 times a day in doses sufficient to completely eliminate the polyuria. However, if fluid intake consistently exceeds replacement needs as evidenced by the development of hyponatremia, the dose should be reduced to allow higher than normal rates of urine output or intermittent breakthrough diuresis. This regimen is often indicated in infants or children because their rate offluid intake tends to be greater than in adults. In all cases, the appropriate dose should be determined by titration, owing to considerable interindividual differences in bioavailability and antidiuretic effect. Conclusions: Desmopressin can provide effective and safe therapy for all patients with neurohy-pophyseal or gestational DI if given in doses and by a route that takes into account the determinants of fluid intake. Copyright © 2013 by The Endocrine Society.