Combined knockout of collecting duct endothelin A and B receptors causes hypertension and sodium retention

doi:10.1152/ajprenal.90279.2008

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Am J Physiol Renal Physiol 295: F1635-F1640, 2008. First published September 10, 2008; doi:10.1152/ajprenal.90279.2008
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Combined knockout of collecting duct endothelin A and B receptors causes hypertension and sodium retention

Yuqiang Ge,¹ Alan Bagnall,² Peter K. Stricklett,¹ David Webb,² Yuri Kotelevtsev,² and Donald E. Kohan¹

¹Division of Nephrology, University of Utah Health Sciences Center, Salt Lake City, Utah; and ²Centre for Cardiovascular Science, University of Edinburgh, Edinburgh, United Kingdom

Submitted 29 April 2008 ; accepted in final form 8 September 2008

The collecting duct (CD) endothelin (ET) system regulates bloodpressure (BP) and Na excretion. CD-specific knockout (KO) ofET-1 causes hypertension, CD-specific KO of the ETA receptordoes not alter BP, while CD-specific KO of the ETB receptorincreases BP to a lesser extent than CD ET-1 KO. These findingssuggest a paracrine role for CD-derived ET-1; however, theydo not exclude compensation for the loss of one ET receptorby the other. To examine this, mice with CD-specific KO of bothETA and ETB receptors were generated (CD ETA/B KO). CD ETA/BKO mice excreted less urinary Na than controls during acuteor chronic Na loading. Urinary aldosterone excretion and plasmarenin concentration were similar during Na intake and both fellcomparably during Na loading. On a normal sodium diet, CD ETA/BKO mice had increased BP, which increased further with highsalt intake. The degree of BP elevation during normal Na intakewas similar to CD ET-1 KO mice and higher than CD ETB KO animals.During 1 wk of Na loading, CD ETA/B KO mice had higher BPs thanCD ETB KO, while BP was less than CD ET-1 KOs until the latterdays of Na loading. These studies suggest that 1) CD ETA/B deficiencycauses salt-sensitive hypertension, 2) CD ETA/B KO-associatedNa retention is associated with failure to suppress the renin-angiotensin-aldosteronesystem, and 3) CD ETA and ETB receptors exerts a combined hypotensiveeffect that exceeds that of either receptor alone.

blood pressure; urinary sodium excretion; cell-specific gene targeting

Address for reprint requests and other correspondence: D. E. Kohan, Division of Nephrology, Univ. of Utah Health Sciences Center, 1900 East, 30 North, Salt Lake City, UT 84132 (e-mail: donald.kohan{at}hsc.utah.edu)