Two Mineralocorticoid Receptor-Mediated Mechanisms of Pendrin Activation in Distal Nephrons

Nobuhiro Ayuzawa; Mitsuhiro Nishimoto; Kohei Ueda; Daigoro Hirohama; Wakako Kawarazaki; Tatsuo Shimosawa; Takeshi Marumo; Toshiro Fujita

doi:10.1681/ASN.2019080804

Two Mineralocorticoid Receptor-Mediated Mechanisms of Pendrin Activation in Distal Nephrons

J Am Soc Nephrol. 2020 Apr;31(4):748-764. doi: 10.1681/ASN.2019080804. Epub 2020 Feb 7.

Authors

Nobuhiro Ayuzawa¹, Mitsuhiro Nishimoto², Kohei Ueda², Daigoro Hirohama², Wakako Kawarazaki², Tatsuo Shimosawa³, Takeshi Marumo², Toshiro Fujita¹

Affiliations

¹ Division of Clinical Epigenetics, Research Center for Advanced Science and Technology, The University of Tokyo, Tokyo, Japan; Toshiro.FUJITA@rcast.u-tokyo.ac.jp ayuzawa-tky@umin.ac.jp.
² Division of Clinical Epigenetics, Research Center for Advanced Science and Technology, The University of Tokyo, Tokyo, Japan.
³ Department of Clinical Laboratory, School of Medicine, International University of Health and Welfare, Chiba, Japan.

Abstract

Background: Regulation of sodium chloride transport in the aldosterone-sensitive distal nephron is essential for fluid homeostasis and BP control. The chloride-bicarbonate exchanger pendrin in β-intercalated cells, along with sodium chloride cotransporter (NCC) in distal convoluted tubules, complementarily regulate sodium chloride handling, which is controlled by the renin-angiotensin-aldosterone system.

Methods: Using mice with mineralocorticoid receptor deletion in intercalated cells, we examined the mechanism and roles of pendrin upregulation via mineralocorticoid receptor in two different models of renin-angiotensin-aldosterone system activation. We also used aldosterone-treated NCC knockout mice to examine the role of pendrin regulation in salt-sensitive hypertension.

Results: Deletion of mineralocorticoid receptor in intercalated cells suppressed the increase in renal pendrin expression induced by either exogenous angiotensin II infusion or endogenous angiotensin II upregulation via salt restriction. When fed a low-salt diet, intercalated cell-specific mineralocorticoid receptor knockout mice with suppression of pendrin upregulation showed BP reduction that was attenuated by compensatory activation of NCC. In contrast, upregulation of pendrin induced by aldosterone excess combined with a high-salt diet was scarcely affected by deletion of mineralocorticoid receptor in intercalated cells, but depended instead on hypokalemic alkalosis through the activated mineralocorticoid receptor-epithelial sodium channel cascade in principal cells. In aldosterone-treated NCC knockout mice showing upregulation of pendrin, potassium supplementation corrected alkalosis and inhibited the pendrin upregulation, thereby lowering BP.

Conclusions: In conjunction with NCC, the two pathways of pendrin upregulation, induced by angiotensin II through mineralocorticoid receptor activation in intercalated cells and by alkalosis through mineralocorticoid receptor activation in principal cells, play important roles in fluid homeostasis during salt depletion and salt-sensitive hypertension mediated by aldosterone excess.

Keywords: aldosterone; angiotensin II; blood pressure; mineralocorticoid receptor; pendrin; sodium chloride cotransporter.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Aldosterone
Animals
Disease Models, Animal
Hypertension / etiology*
Mice
Mice, Knockout
Nephrons / metabolism*
Nephrons / pathology*
Receptors, Mineralocorticoid / physiology*
Renin-Angiotensin System / physiology
Sodium Chloride Symporters / physiology*
Sulfate Transporters / metabolism*

Substances

Receptors, Mineralocorticoid
Slc26a4 protein, mouse
Sodium Chloride Symporters
Sulfate Transporters
Aldosterone