Polymorphisms in the carboxy-terminus of the epithelial sodium channel in rat models for hypertension : Journal of Hypertension

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Original article

Polymorphisms in the carboxy-terminus of the epithelial sodium channel in rat models for hypertension

Gründer, Stefan1; Zagato, Laura2; Yagil, Chana3; Yagil, Yoram3; Sassard, Jean4; Rossier, Bernard C.1

Author Information

1From the Institut de Pharmacologie et de Toxicologie de l'Université, Lausanne, Switzerland

2Division of Nephrology, Dialysis and Hypertension, University of Milan, San Raffaele Hospital, Milan, Italy

3Barzilai Medical Center – Ashkelon, Faculty of Health Sciences, Ben-Gurion University, Israel

4Département de Physiologie et de la Pharmacologie Clinique, Faculté de Pharmacie, Lyon, France. S.G. and L.Z. contributed equally to this work.

Sponsorship: This study was supported by grant 31-43384.95 from the Swiss National Fund for Scientific Research to B.C.R. and by EURHYPGEN Concerted Action of the European Commission to the laboratory of L.Z.

Requests for reprints to Bernard C. Rossier, Institut de Pharmacologie et de Toxicologie de l'Université, Rue du Bugnon 27, CH-1005 Lausanne, Switzerland.

Received 31 May 1996 Revised 3 October 1996 Accepted 22 November 1996

Journal of Hypertension 15(2):p 173-179, February 1997.

Abstract

Objective 

To investigate whether mutations in the C-terminus of the three subunits of the rat epithelial sodium channel (αβγ-rENaC) contribute to the hypertensive phenotype in five rat models for essential hypertension.

Design 

We sequenced the C-terminal regions of α-, β- and γ-rENaC genes in five different hypertensive rat strains [spontaneously hypertensive rats (SHR), Dahl salt-sensitive (SS/Jr) rats, Milan hypertensive (MHS) rats, Sabra hypertensive (SBH) rats and Lyon hypertensive rats (LHR)] and their normotensive controls [Wistar–Kyoto (WKY) rats, Dahl salt-resistant (SR/Jr) rats, Milan normotensive (MNS) rats, Sabra normotensive (SBN) rats and Lyon normotensive rats (LNR)]. Identified polymorphisms were tested for cosegregation with blood pressure as well as for increased epithelial sodium channel (ENaC) activity.

Methods 

Genomic DNA extracted from hypertensive and normotensive rat strains was amplified by the polymerase chain reaction and polymerase chain reaction fragments were sequenced. Cosegregation analysis was performed to test for correlations between blood pressure and different genotypes. The effects of a polymorphism on ENaC activity were assessed by functional expression in Xenopus laevis oocytes. The chromosomal location of the gene for γ-ENaC was determined by linkage analysis in an F2 (MHS × MNS) population.

Results 

We found no polymorphisms at the C-terminus of α- and β-rENaC in the five rat models tested. We identified two polymorphisms at the C-terminus of the γ-subunit, one leading to an amino acid change. Milan strains (MNS and MHS) were polymorphic for this mutation. By cosegregation analysis we could exclude the possibility that there was a correlation between blood pressure and this polymorphism. Functional expression of the polymorphism caused no increase in ENaC activity assessed by measurement of the amiloride-sensitive sodium current in Xenopus oocytes. The gene for the γ-ENAC was located on rat chromosome 1.

Conclusions 

No polymorphisms at the C-terminus of the three subunits of the epithelial sodium channel cosegregating with blood pressure were detected in five different genetic rat models for hypertension. If an altered ENaC activity contributes to the pathogenesis of hypertension in these rats, it must thus arise from mutations in other parts of the protein, from mutations outside the coding region impairing the proper regulation of one of the subunits or from mutations in an ENaC-associated protein.

© Lippincott-Raven Publishers.

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