NADPH Oxidase in the Renal Medulla Causes Oxidative Stress and Contributes to Salt-sensitive Hypertension in Dahl S Rats

Overview

Journal Hypertension

Date 2006 Mar 1

PMID 16505210

Citations 107

Authors

Norman E Taylor

Padden Glocka

Mingyu Liang

Allen W Cowley Jr

Affiliations

Soon will be listed here.

Abstract

Dahl salt-sensitive (SS) rats exhibit increased renal medullary oxidative stress and blood pressure salt-sensitivity compared with consomic, salt-resistant SS-13BN rats, despite highly similar genetic backgrounds. The present study examined potential sources of renal medullary superoxide in prehypertensive SS rats fed a 0.4% NaCl diet by assessing activity and protein levels of superoxide producing and scavenging enzymes. Superoxide production was nearly doubled in SS rats compared with SS-13BN rats as determined by urinary 8-isoprostane excretion and renal medullary oxy-ethidium microdialysate levels. Medullary superoxide production in tissue homogenates was greater in SS rats, and the NADPH oxidase inhibitor diphenylene iodonium preferentially reduced SS levels to those found in SS-13BN rats. Dinitrophenol, a mitochondrial uncoupler, eliminated the remaining superoxide production in both strains, whereas inhibition of xanthine oxidase, NO synthase, and cycloxygenase had no effect. L-arginine, NO synthase, superoxide dismutase, catalase, and glutathione peroxidase activities between SS and SS-13BN rats did not differ. Chronic blood pressure responses to a 4% NaCl diet were then determined in the presence or absence of the NADPH oxidase inhibitor apocynin (3.5 microg/kg per minute), chronically delivered directly into the renal medulla. Apocynin infusion reduced renal medullary interstitial superoxide from 1059+/-130 to 422+/-80 (oxyethidium fluorescence units) and mean arterial pressure from 175+/-4 to 157+/-6 mm Hg in SS rats, whereas no effects on either were observed in the SS-13(BN). We conclude that excess renal medullary superoxide production in SS rats contributes to salt-induced hypertension, and NADPH oxidase is the major source of the excess superoxide.

Citing Articles

Renal Medulla in Hypertension.

Cowley Jr A, Roman R, Mattson D, Franchini K, OConnor P, Makino A Hypertension. 2024; 81(12):2383-2394.

PMID: 39344517 PMC: 11578791. DOI: 10.1161/HYPERTENSIONAHA.124.21711.

Renal Epithelial Mitochondria: Implications for Hypertensive Kidney Disease.

Stadler K, Ilatovskaya D Compr Physiol. 2023; 14(1):5225-5242.

PMID: 38158371 PMC: 11194858. DOI: 10.1002/cphy.c220033.

8-Aminopurines in the Cardiovascular and Renal Systems and Beyond.

Jackson E, Tofovic S, Chen Y, Birder L Hypertension. 2023; 80(11):2265-2279.

PMID: 37503660 PMC: 10592300. DOI: 10.1161/HYPERTENSIONAHA.123.20582.

Descending Control of Nociception Poorly Predicts the Development of Persistent Postsurgical Pain-like Behavior in Consomic Dahl S Rat Strains.

Ferrari L, Wilkinson A, Cahoon C, Ramirez A, Rey C, Donaldson G Anesthesiology. 2023; 139(4):476-491.

PMID: 37351557 PMC: 10530067. DOI: 10.1097/ALN.0000000000004662.

Functional NADPH oxidase 2 in T cells amplifies salt-sensitive hypertension and associated renal damage.

Walton S, Dasinger J, Burns E, Cherian-Shaw M, Abais-Battad J, Mattson D Am J Physiol Renal Physiol. 2023; 325(2):F214-F223.

PMID: 37318993 PMC: 10396224. DOI: 10.1152/ajprenal.00014.2023.