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Am J Physiol Cell Physiol 277: C461-C468, 1999;
0363-6143/99 $5.00
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Vol. 277, Issue 3, C461-C468, September 1999

Angiotensin regulates the selectivity of the Na+-K+ pump for intracellular Na+

Kerrie A. Buhagiar1,2, Peter S. Hansen1,2, David F. Gray1,2, Anastasia S. Mihailidou1, and Helge H. Rasmussen1,2

1 Department of Cardiology, Royal North Shore Hospital, St. Leonards 2065; and 2 University of Sydney, Sydney, New South Wales 2006, Australia

Treatment of rabbits with angiotensin-converting enzyme (ACE) inhibitors increases the apparent affinity of the Na+-K+ pump for Na+. To explore the mechanism, we voltage clamped myocytes from control rabbits and rabbits treated with captopril with patch pipettes containing 10 mM Na+. When pipette solutions were K+ free, pump current (Ip) for myocytes from captopril-treated rabbits was nearly identical to that for myocytes from controls. However, treatment caused a significant increase in Ip measured with pipettes containing K+. A similar difference was observed when myocytes from rabbits treated with the ANG II receptor antagonist losartan and myocytes from controls were compared. Treatment-induced differences in Ip were eliminated by in vitro exposure to ANG II or phorbol 12-myristate 13-acetate or inclusion of the protein kinase C fragment composed of amino acids 530-558 in pipette solutions. Treatment with captopril had no effect on the voltage dependence of Ip. We conclude that ANG II regulates the pump's selectivity for intracellular Na+ at sites near the cytoplasmic surface. Protein kinase C is implicated in the messenger cascade.

cardiac myocytes; sodium; protein kinase C


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