Reduced ENaC protein abundance contributes to the lower blood pressure observed in pendrin-null mice

Pendrin (encoded by Pds, Slc26a4) is a Cl−/HCO3− exchanger expressed in the apical regions of type B and non-A, non-B intercalated cells of kidney and mediates renal Cl− absorption, particularly when upregulated. Aldosterone increases blood pressure by increasing absorption of both Na+ and Cl− through increased protein abundance and function of Na+ transporters, such as the epithelial Na+ channel (ENaC) and the Na+-Cl− cotransporter (NCC), as well as Cl− transporters, such as pendrin. Because aldosterone analogs do not increase blood pressure in Slc26a4−/− mice, we asked whether Na+ excretion and Na+ transporter protein abundance are altered in kidneys from these mutant mice. Thus wild-type and Slc26a4-null mice were given a NaCl-replete, a NaCl-restricted, or NaCl-replete diet and aldosterone or aldosterone analogs. Abundance of the major renal Na+ transporters was examined with immunoblots and immunohistochemistry. Slc26a4-null mice showed an impaired ability to conserve Na+ during dietary NaCl restrict...