Development of Lithium-induced Nephrogenic Diabetes Insipidus is Dissociated from Adenylyl Cyclase Activity

Overview

Journal J Am Soc Nephrol

Specialty Nephrology

Date 2006 Feb 24

PMID 16495377

Citations 40

Authors

Yuedan Li

Stephen Shaw

Erik-Jan Kamsteeg

Alain Vandewalle

Peter M T Deen

Affiliations

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Abstract

In antidiuresis, vasopressin (AVP) occupation of V2 receptors in renal collecting ducts activates adenylyl cyclase, resulting in increased intracellular cAMP levels, which activates protein kinase A (PKA). PKA phosphorylates both the cAMP responsive element binding protein, which induces aquaporin-2 (AQP2) transcription, and AQP2, which then is translocated to the apical membrane, allowing urine concentration. Lithium treatment often causes nephrogenic diabetes insipidus (NDI), which coincides with decreased AQP2 expression and which generally is ascribed to reduced adenylyl cyclase activity. However, the underlying mechanism by which lithium causes NDI is poorly understood. This study demonstrated that the mouse cortical collecting duct mpkCCD(c14) cells are a good model; the deamino-8 D-arginine vasopressin (dDAVP)-induced endogenous AQP2 expression and plasma membrane localization was time-dependently reduced by treatment with clinically relevant lithium concentrations. Lithium did not affect AQP2 stability but decreased its mRNA levels. Surprising, the effect of lithium was cAMP independent; it did not alter AVP-stimulated cAMP production or PKA-dependent phosphorylation of AQP2 or cAMP responsive element binding protein. In vivo, kidney tissue of rats with lithium-induced NDI indeed generated less dDAVP-induced cAMP than that of controls, but this could be due to elevated blood AVP levels in rats with lithium-induced NDI. Indeed, Brattleboro rats, which lack endogenous AVP, with clamped blood dDAVP levels, showed no difference in dDAVP-generated cAMP generation between kidneys of rats with lithium-induced NDI and control rats. In conclusion, the first proper cell model to study lithium-induced NDI was developed, and it was demonstrated that the lithium-induced downregulation of AQP2 and development of NDI occur independent of adenylyl cyclase activity in vitro and in vivo.

Citing Articles

Central Diabetes Insipidus in the Background of Lithium Use: Consider Central Causes Despite Nephrogenic as the Most Common.

Li J, Tan S, Kawashita T, Tagle C, Farmand F Am J Case Rep. 2023; 24:e939034.

PMID: 36683312 PMC: 9883600. DOI: 10.12659/AJCR.939034.

Lithium Biological Action Mechanisms after Ischemic Stroke.

Munteanu C, Rotariu M, Turnea M, Tataranu L, Dogaru G, Popescu C Life (Basel). 2022; 12(11).

PMID: 36362835 PMC: 9697783. DOI: 10.3390/life12111680.

A Vasopressin-Induced Change in Prostaglandin Receptor Subtype Expression Explains the Differential Effect of PGE on AQP2 Expression.

Deen P, Boone M, Schweer H, Olesen E, Carmone C, Wetzels J Front Physiol. 2022; 12:787598.

PMID: 35126177 PMC: 8814457. DOI: 10.3389/fphys.2021.787598.

Reduced risk for hospitalization due to hyponatraemia in lithium treated patients: A Swedish population-based case-control study.

Falhammar H, Skov J, Calissendorff J, Lindh J, Mannheimer B J Psychopharmacol. 2020; 35(2):184-189.

PMID: 32684112 PMC: 7859672. DOI: 10.1177/0269881120937597.

Lithium Chloride and GSK3 Inhibition Reduce Aquaporin-2 Expression in Primary Cultured Inner Medullary Collecting Duct Cells Due to Independent Mechanisms.

Kaiser M, Edemir B Cells. 2020; 9(4).

PMID: 32340354 PMC: 7226097. DOI: 10.3390/cells9041060.