Angiotensin II-induced contraction is attenuated by nitric oxide in afferent arterioles from the nonclipped kidney in 2K1C

Helle, Frank; Hultström, Michael; Skogstrand, Trude; Palm, Fredrik; Iversen, Bjarne M.

doi:10.1152/ajprenal.90518.2008

Cited by 26 publications

(39 citation statements)

References 31 publications

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“…We concluded that Ang II activates PI3K/ Akt1 via the AT 2 receptors, inducing phosphorylation of NOS3 at serines 1177 and 633, resulting in increased production of NO by the TAL. NO has been shown to buffer the actions of Ang II within the renal medulla (5,(45)(46)(47)(48)(49). In the TAL, NO inhibits (15,50), reabsorption whereas O 2 Ϫ stimulates Na ϩ reabsorption (51).…”

Section: Discussionmentioning

confidence: 99%

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

Herrera

Garvin

2010

Journal of Biological Chemistry

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Ang II increased phospho-NOS3 at serine 1177 by 130% (p < 0.01) and 150% after 5 and 10 min (p < 0.02). Ang II increased phosphoNOS3 at serine 633 by 50% after 5 min (p < 0.01). Akt inhibition prevented NOS3 phosphorylation. We concluded that Ang II enhances TAL NO production via activation of AT 2 and Akt1-dependent phosphorylation of NOS3 at serines 1177 and 633. The thick ascending limb (TAL)2 of the loop of Henle is the diluting segment of the renal nephron. It reabsorbs ϳ30% of filtered NaCl and generates the osmotic gradient necessary for water reabsorption by the collecting duct. Enhanced Na ϩ reabsorption by this segment has been implicated in the development of hypertension (1, 2). The TAL cells produce NO. Endogenously produced NO inhibits Na ϩ reabsorption by the TAL (3, 4). Inappropriate NO bioavailability can lead to enhanced TAL Na ϩ reabsorption, Na ϩ retention, and hypertension. Thus, understanding the signaling cascade leading to NO production by TALs could help understand the pathophysiology of hypertension and identify new targets for its treatment.In the TAL, NO is stimulated by a number of factors including angiotensin II (Ang II) (5). Ang II can activate two different receptors: type 1 (AT 1 ) or type 2 (AT 2 ). In the vasculature, activation of AT 1 leads to vasoconstriction, resulting in increased renal vascular resistance (6). In contrast, activation of AT 2 in endothelial cells stimulates NO release (7). Similarly, in the kidney, activation of AT 1 mediates the salt-retaining and prohypertensive actions of Ang II (8 -12), whereas activation of AT 2 leads to natriuresis via activation of the NO/cGMP signaling pathway (13, 14). To our knowledge, the receptor that mediates the stimulatory actions of Ang II on NO production by the TAL has not yet been identified.In the TAL, NO is produced by nitric-oxide synthase 3 (NOS3 or eNOS) (15, 16). NOS3 can be activated by several signaling pathways, including those involving Ca 2ϩ /calmodulin (17) and Akt-dependent phosphorylation of NOS3 (18,19). In endothelial cells, both pathways are important. However, in epithelial cells, activation of Akt appears to be the main mechanism (20). Three Akt isoforms have been identified: Akt1, -2, and -3. In endothelial cells, Akt1 directly phosphorylates NOS3 at serine 1177, heightening enzyme activity and NO production (18,(21)(22)(23)(24)(25). In the TAL, activation of Akt has been shown to participate in the activation of NOS3 by different stimuli (16,20,26,27,28). However, the mechanism by which Ang II stimulates NO in the TAL has not been investigated to our knowledge. We hypothesized that Ang II stimulates TAL NO production via activation of AT 2 and Akt1, phosphorylating NOS3 at serine 1177 and enhancing NO production. EXPERIMENTAL PROCEDURES

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Section: Discussionmentioning

confidence: 99%

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

Herrera

Garvin

2010

Journal of Biological Chemistry

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“…Combined inhibition of nitric oxide synthesis and ANG II stimulation uncovers a decreased contractility and almost no nitric oxide production in vessel preparations from animals with heart failure (26). This shows a marked difference from the effect of ANG II on afferent arterioles in high renin hypertension models (22,24) and during ANG II blockade in vivo (61). ANG II increases tubular sodium reabsorption (47), although reabsorption may be decreased by ANG II in the proximal nephron (37,64).…”

Section: Renin-angiotensinmentioning

confidence: 96%

Renal neurohormonal regulation in heart failure decompensation

Jönsson

Becirovic‐Agic

Narfström

et al. 2014

American Journal of Physiology-Regulatory, Integrative and Comp

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“…ANG II is a key hormone in the regulation of RBF and GFR. However, its effect is in many situations balanced by vasodilators such as vasodilatory prostanoids and nitric oxide (NO) (6). Together these signaling substances are of major importance in the regulation of RBF in the normal kidney and probably more so in hypertensive models where the components of the reninangiotensin system are activated or increased.…”

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confidence: 99%

“…We have recently shown that ANG II-induced NO release controls renal vascular resistance by its ability to adjust the diameter of preglomerular vessels in the nonclipped kidney of two-kidney, one-clip hypertensive (2K1C) animals (6). The nonclipped kidney is subjected to high perfusion pressure and high vascular NO release, while vascular NO production is low in the clipped kidney.…”

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confidence: 99%

AT₁ receptor activation regulates the mRNA expression of CAT1, CAT2, arginase-1, and DDAH2 in preglomerular vessels from angiotensin II hypertensive rats

Hultström

Helle²,

Iversen³

2009

American Journal of Physiology-Renal Physiology

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Hultström M, Helle F, Iversen BM. AT1 receptor activation regulates the mRNA expression of CAT1, CAT2, arginase-1, and DDAH2 in preglomerular vessels from angiotensin II hypertensive rats. Am J Physiol Renal Physiol 297: F163-F168, 2009. First published April 22, 2009 doi:10.1152/ajprenal.00087.2009.-Previously, we found increased expression of L-arginine metabolizing enzymes in both kidneys from two-kidney, one-clip (2K1C) hypertensive rats (Helle F, Hultstrom M, Skogstrand T, Palm F, Iversen BM. Am J Physiol Renal Physiol 296: F78 -F86, 2009). In the present study, we investigate whether AT 1 receptor activation can induce the changes observed in 2K1C. Four groups of rats were infused with 80 ng/min ANG II or saline for 14 days and/or given 60 mg ⅐ kg Ϫ1 ⅐ day Ϫ1losartan. Gene expression was studied in isolated preglomerular vessels by RT-PCR. Dose-responses to ANG II were studied in isolated preglomerular vessels with and without acute NOS inhibition [10Expressions of endothelial nitric oxide synthase (eNOS), caveolin-1, and arginase-2 were not changed by ANG II infusion. CAT1 (0.3 8 Ϯ 0.07 to 0.73 Ϯ 0.12, P Ͻ 0.05), CAT2 (1.14 Ϯ 0.29 to 2.74 Ϯ 0.48), DDAH2 (1.09 Ϯ 0.27 to 2.3 Ϯ 0.46), and arginase-1 (1.08 Ϯ 0.17 to 1.82 Ϯ 0.22) were increased in ANG II-infused rats. This was prevented by losartan treatment, which reduced the expression of eNOS (0.97 Ϯ 0.26 to 0.37 Ϯ 0.11 in controls; 0.8 Ϯ 0.16 to 0.36 Ϯ 0.1 in ANG II-infused rats) and caveolin-1 (2.49 Ϯ 0.59 to 0.82 Ϯ 0.24 in controls and 2.59 Ϯ 0.61 to 1.1 Ϯ 0.25 in ANG II-infused rats). ANG II (10 Ϫ10 mol/l) caused vessels from ANG II-infused animals to contract to 53 Ϯ 15% of baseline diameter and 90 Ϯ 5% of baseline diameter in controls (P Ͻ 0.05) and was further enhanced by L-NAME to 4 Ϯ 4% of baseline diameter (P Ͻ 0.05). In vivo losartan treatment reduced the reactivity of isolated vessels to 91 Ϯ 2% of baseline in response to 10 Ϫ7 mol/l ANG II compared with 82 Ϯ 3% in controls (P Ͻ 0.05) and prevented the increased responsiveness caused by ANG II infusion. In conclusion, CAT1, CAT2, DDAH2, and arginase-1 expression in renal resistance vessels is regulated through the AT 1 receptor. This finding may be of direct importance for NOS and the regulation of preglomerular vascular function.caveolin-1; afferent arteriole; contraction; losartan THE AFFERENT ARTERIOLES (AAs) are the main site for regulation of renal blood flow (RBF) and glomerular filtration rate (GFR). This control is mediated by three main mechanisms: first, hormonal factors (endocrine, autocrine or paracrine); second, the sympathetic nervous system; and third, the myogenic and tubuloglomerular feedback systems (11). ANG II is a key hormone in the regulation of RBF and GFR. However, its effect is in many situations balanced by vasodilators such as vasodilatory prostanoids and nitric oxide (NO) (6). Together these signaling substances are of major importance in the regulation of RBF in the normal kidney and probably more so in hypertensive models where the components of the reninangiotensi...

show abstract

Angiotensin II-induced contraction is attenuated by nitric oxide in afferent arterioles from the nonclipped kidney in 2K1C

Cited by 26 publications

References 31 publications

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

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

Renal neurohormonal regulation in heart failure decompensation

AT₁ receptor activation regulates the mRNA expression of CAT1, CAT2, arginase-1, and DDAH2 in preglomerular vessels from angiotensin II hypertensive rats

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