Angiotensin II Stimulates Thick Ascending Limb NO Production via AT2 Receptors and Akt1-dependent Nitric-oxide Synthase 3 (NOS3) Activation

Herrera, Marcela; Garvin, Jeffrey L.

doi:10.1074/jbc.m110.109041

Cited by 33 publications

(28 citation statements)

References 53 publications

(71 reference statements)

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“…production in human platelets, and this effect was blunted by an AT 1 receptor antagonist. Although we recently reported that Ang II acts on AT 2 receptors to activate other signaling events in the TAL (34), in the present study the AT 2 antagonist PD123319 had no effect on Ang II-stimulated O 2 . production, suggesting that AT 2 receptors do not play a role in AT 1 -stimulated O 2 .…”

Section: Angiotensin Stimulates Tal Ocontrasting

confidence: 83%

Angiotensin II Stimulates Thick Ascending Limb Superoxide Production via Protein Kinase Cα-dependent NADPH Oxidase Activation

Herrera

Silva

Garvin

2010

Journal of Biological Chemistry

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Section: Angiotensin Stimulates Tal Ocontrasting

confidence: 83%

Angiotensin II Stimulates Thick Ascending Limb Superoxide Production via Protein Kinase Cα-dependent NADPH Oxidase Activation

Herrera

Silva

Garvin

2010

Journal of Biological Chemistry

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“…In view of the results obtained during the high-and low-salt diets, we supposed that angiotensin II might be involved in regulating the differential splicing of NKCC2. Both the AT 1 and AT 2 receptors have been shown to be expressed in the TAL and to be relevant for TAL function (14,15,24,30). Our experiments showed that chronic angiotensin II infusion led to a shift in the expression of NKCC2 from the A isoform to the B isoform similar to that which occurred for dietary salt restriction, and this regulation was most obvious in the renal cortex.…”

Section: Discussionsupporting

confidence: 55%

Dietary salt intake modulates differential splicing of the Na-K-2Cl cotransporter NKCC2

Schieβl

Rosenauer

Kattler

et al. 2013

American Journal of Physiology-Renal Physiology

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Schie␤l IM, Rosenauer A, Kattler V, Minuth WW, Oppermann M, Castrop H. Dietary salt intake modulates differential splicing of the Na-K-2Cl cotransporter NKCC2. Am J Physiol Renal Physiol 305: F1139 -F1148, 2013. First published August 14, 2013 doi:10.1152/ajprenal.00259.2013.-Both sodium reabsorption in the thick ascending limb of the loop of Henle (TAL) and macula densa salt sensing crucially depend on the function of the Na/K/2Cl cotransporter NKCC2. The NKCC2 gene gives rise to at least three different full-length NKCC2 isoforms derived from differential splicing. In the present study, we addressed the influence of dietary salt intake on the differential splicing of NKCC2. Mice were subjected to diets with low-salt, standard salt, and high-salt content for 7 days, and NKCC2 isoform mRNA abundance was determined. With decreasing salt intake, we found a reduced abundance of the low-affinity isoform NKCC2A and an increase in the high-affinity isoform NKCC2B in the renal cortex and the outer stripe of the outer medulla. This shift from NKCC2A to NKCC2B during a low-salt diet could be mimicked by furosemide in vivo and in cultured kidney slices. Furthermore, the changes in NKCC2 isoform abundance during a salt-restricted diet were partly mediated by the actions of angiotensin II on AT 1 receptors, as determined using chronic angiotensin II infusion. In contrast to changes in oral salt intake, water restriction (48 h) and water loading (8% sucrose solution) increased and suppressed the expression of all NKCC2 isoforms, without changing the distribution pattern of the single isoforms. In summary, the differential splicing of NKCC2 pre-mRNA is modulated by dietary salt intake, which may be mediated by changes in intracellular ion composition. Differential splicing of NKCC2 appears to contribute to the adaptive capacity of the kidney to cope with changes in reabsorptive needs. differential spacing; NKCC2; salt transport THE THICK ASCENDING LIMB OF the loop of Henle (TAL) contributes to 25-30% of total renal Na ϩ reabsorption. Apical Na uptake in cells of the TAL is primarily mediated by the bumetanide-sensitive Na-K-2Cl cotransporter NKCC2 (5). In addition to its function in TAL salt retrieval, the NKCC2-dependent transport activity of macula densa cells constitutes the initial step in the tubulovascular signaling pathways between the TAL in the juxtaglomerular region and the afferent arteriole (20,33). By detecting changes in luminal NaCl concentration, macula densa cells modulate the tone of the afferent arteriole and subsequently control the single-nephron glomerular filtration rate. This negative feedback loop is known as tubuloglomerular feedback (TGF; Ref. 38). Macula densa cells also control the secretion of renin from granular cells of the afferent arteriole (4).NKCC2 is encoded by the gene Slc12a1 (8, 16). In humans and all other examined mammalian species, differential splicing of Slc12a1 gives rise to at least three different full-length isoforms of NKCC2, known as NKCC2B, NKCC2A, and NKCC2F (3,16,28,40). ...

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“…Phosphorylation at Ser1177 of NOS3 is regulated by Akt kinase activation (13,28,36), while ANG II increases Akt phosphorylation at Ser473 in renal thick ascending limb (15). Thus we analyzed total and phosphorylated Akt at Ser473 in small mesenteric arteries from NORM and ANG rats (n ϭ 7; Fig.…”

Section: Resultsmentioning

confidence: 99%

Antihypertensive therapy increases tetrahydrobiopterin levels and NO/cGMP signaling in small arteries of angiotensin II-infused hypertensive rats

Kang

Sullivan

Spradley

et al. 2011

American Journal of Physiology-Heart and Circulatory Physiology

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We previously reported that small mesenteric arteries from hypertensive rats have increased NOS-derived H(2)O(2) and reduced NO/cGMP signaling. We hypothesized that antihypertensive therapy lowers blood pressure through a tetrahydrobiopterin (BH(4))-dependent mechanism restoring NO/cGMP signaling and endothelial NOS (NOS3; eNOS) phosphorylation in small arteries. To test this hypothesis, small mesenteric arteries from normotensive rats (NORM), angiotensin II-infused rats (ANG), ANG rats with triple therapy (reserperine, hydrochlorothiazide, and hydralazine), or ANG rats with oral BH(4) therapy were studied. Both triple therapy and oral BH(4) therapy attenuated the rise in systolic blood pressure in ANG rats and restored NO/cGMP signaling in small arteries similarly. Triple therapy significantly increased vascular BH(4) levels and BH(4)-to-BH(2) ratio similar to ANG rats with BH(4) supplementation. Furthermore, triple therapy (but not oral BH(4) therapy) significantly increased GTP cyclohydrolase I (GTPCH I) activity in small arteries without a change in expression. NOS3 phosphorylation at Ser1177 was reduced in small arteries from ANG compared with NORM, while NOS3 phosphorylation at Ser633 and Thr495 were similar in ANG and NORM. NOS3 phosphorylation at Ser1177 was restored with triple therapy or oral BH(4) in ANG rats. In conclusion, antihypertensive therapy regulates NO/cGMP signaling in small arteries through increasing BH(4) levels and NOS3 phosphorylation at Ser1177.

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Angiotensin II Stimulates Thick Ascending Limb NO Production via AT2 Receptors and Akt1-dependent Nitric-oxide Synthase 3 (NOS3) Activation

Cited by 33 publications

References 53 publications

Angiotensin II Stimulates Thick Ascending Limb Superoxide Production via Protein Kinase Cα-dependent NADPH Oxidase Activation

Angiotensin II Stimulates Thick Ascending Limb Superoxide Production via Protein Kinase Cα-dependent NADPH Oxidase Activation

Dietary salt intake modulates differential splicing of the Na-K-2Cl cotransporter NKCC2

Antihypertensive therapy increases tetrahydrobiopterin levels and NO/cGMP signaling in small arteries of angiotensin II-infused hypertensive rats

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