Female ROMK null mice manifest more severe Bartter II phenotype on renal function and higher PGE2 production

doi:10.1152/ajpregu.00051.2007

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Am J Physiol Regul Integr Comp Physiol 295: R997-R1004, 2008. First published June 25, 2008; doi:10.1152/ajpregu.00051.2007
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WATER AND ELECTROLYTE HOMEOSTASIS

Female ROMK null mice manifest more severe Bartter II phenotype on renal function and higher PGE₂ production

Qingshang Yan, Xinbo Yang, Alessandra Cantone, Gerhard Giebisch, Steven Hebert, and Tong Wang

Department of Cellular and Molecular Physiology, Yale University School of Medicine, New Haven, Connecticut

Submitted 24 January 2007 ; accepted in final form 21 June 2008

ROMK null mice with a high survival rate and varying severityof hydronephrosis provide a good model to study type II Barttersyndrome pathophysiology (26). During the development of sucha colony, we found that more male than female null mice survived,58.7% vs. 33.3%. To investigate the possible mechanism of thisdifference, we compared the survival rates, renal functions,degree of hydronephrosis, as well as PGE₂ and TXB₂ productionbetween male and female ROMK wild-type and null mice. We observedthat female ROMK Bartter's mice exhibited lower GFR (0.37 vs.0.54 ml·min^–1·100 g BW^–1, P < 0.05)and higher fractional Na⁺ excretion (0.66% vs. 0.48%, P <0.05) than male Bartter's. No significant differences in acid-baseparameters, urinary K⁺ excretion, and plasma electrolyte concentrationswere observed between sexes. In addition, we assessed the liquidretention rate in the kidney to evaluate the extent of hydronephrosisand observed that 67% of male and 90% of female ROMK null micewere hydronephrotic mice. Urinary PGE₂ excretion was higherin both sexes of ROMK null mice: 1.35 vs. 1.10 ng/24 h in malesand 2.90 vs. 0.87 ng/24 h in females. TXB₂ excretion was higherin female mice in both wild-type and ROMK null mice. The incrementsof urinary PGE₂ and TXB₂ were significantly higher in femalenull mice than males, 233.33% vs. 22.74% of PGE₂ and 85.67%vs. 20.36% of TXB₂. These data demonstrate a more severe Bartterphenotype in female ROMK null mice, and higher PGE₂ and TXB₂production may be one of the mechanisms of this manifestation.

gender difference; ROMK Bartter's; hydronephrosis; renal function

Address for reprint requests and other correspondence: T. Wang, Dept. of Cellular and Molecular Physiology, Yale Univ. School of Medicine, 333 Cedar St., New Haven, CT 06520 (e-mail: tong.wang{at}yale.edu)