Evidence for the involvement of different receptor subtypes in the pre‐ and postjunctional actions of angiotensin II at rat sympathetic neuroeffector sites

Cox, Sandra; Ben, A.; Story, D. F.; Ziogas, James

doi:10.1111/j.1476-5381.1995.tb13313.x

Cited by 47 publications

(60 citation statements)

References 25 publications

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“…The significantly greater basal luminal perfusion pressure observed in the present study in caudal artery preparations from SH rats compared to that in preparations from WKY rats is consistent with findings with the mesenteric vasculature (Lais & Brody, 1978; tions of angiotensin II in rabbit renal artery (Zhang et al, 1994), rat portal vein, rabbit aorta and pulmonary artery (Rhaleb et al, 1991). Likewise, we previously described blockade by losartan of the vasoconstrictor response to angiotensin II in the caudal artery of Sprague-Dawley rats (Cox et al, 1995 Prejuncdonal anglotensin 11 receptors in SH rats sponse. In preparations from both strains of rats, the maximal enhancement of S-I [3H]-noradrenaline efflux and of the vasoconstrictor response occurred with a concentration of 1 gM and a further increase in concentration to 3 gM produced less enhancement.…”

Section: Discussionsupporting

confidence: 80%

“…We have recently found that the enhancement of transmitter noradrenaline release by angiotensin II in the caudal artery of Sprague-Dawley rats is blocked by both losartan and PD 123319 (Cox et al, 1995). Thus, we suggested that the prejunctional receptor subserving the enhancement of transmitter noradrenaline release in this tissue had characteristics similar to the ATIB binding site described by Zhou et al (1993).…”

Section: Introductionmentioning

confidence: 59%

“…Thus, we suggested that the prejunctional receptor subserving the enhancement of transmitter noradrenaline release in this tissue had characteristics similar to the ATIB binding site described by Zhou et al (1993). In contrast, the receptor subtype subserving the direct vasoconstrictor actions of angiotensin II in the rat caudal artery was found to be sensitive to losartan but not PD 123319 (Cox et al, 1995), which is consistent with results from other studies (Rhaleb et al, 1991).In our studies with isolated caudal artery preparations from a normotensive (Sprague-Dawley) strain of rat, we found that, compared to published findings in other tissues, angiotensin II had a relatively low potency in respect of its ability to enhance stimulation-induced (S-I) [3H]-noradrenaline efflux (Cox et al, 1996). In addition, a striking and unexpected finding of those studies was that the enhancement of S-I [3H]-noradrenaline efflux and of the associated vasoconstrictor responses produced by angiotensin II, in a concentration just above threshold (0.1 /iM), was greatly increased in the presence of 0.01 gM losartan.…”

mentioning

confidence: 91%

“…Angiotensin II-mediated effects such as vascular smooth muscle contraction (Cox et al, 1995), aldosterone release (Wong et al, 1990a) and the regulation of fluid and electrolyte balance (Barbella et al, 1993) are all blocked by losartan and unaffected by AT2 receptor antagonists. Hence, the major physiological actions of angiotensin II appear to involve the AT1 receptor subtype and a functional role of the AT2 receptor remains to be determined.…”

Section: Introductionmentioning

confidence: 99%

“…Thus, two populations of AT, sites on mesangial cells were shown to bind losartan and PD 123319 with different relative affinities Madhun et al, 1993). The sites for which losartan had the higher affinity were classified ATlA and those for which PD 123319 had the higher affinity were termed ATIB .Angiotensin II-mediated effects such as vascular smooth muscle contraction (Cox et al, 1995), aldosterone release (Wong et al, 1990a) and the regulation of fluid and electrolyte balance (Barbella et al, 1993) are all blocked by losartan and unaffected by AT2 receptor antagonists. Hence, the major physiological actions of angiotensin II appear to involve the AT1 receptor subtype and a functional role of the AT2 receptor remains to be determined.…”

mentioning

confidence: 99%

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Angiotensin II receptors involved in the enhancement of noradrenergic transmission in the caudal artery of the spontaneously hypertensive rat

Cox

Story

Ziogas

1996

British J Pharmacology

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1 The effects of the AT, receptor antagonist losartan and the AT2 receptor antagonist PD 123319, on actions of angiotensin II in isolated caudal arteries of spontaneously hypertensive (SH) and age-matched normotensive (Wistar-Kyoto) rats were compared.2 Angiotensin II (0.1-3 gM) produced concentration-dependent increases in perfusion pressure in artery preparations from both SH and Wistar-Kyoto (WKY) rats, the maximal increase in the SH rat being significantly greater than the increase in WKY rats. The increase in perfusion pressure in preparations from both strains of rats was prevented by losartan (0.1 /M) and unaffected by PD 123319 (0.1 uM), indicating that the vasoconstrictor action of angiotensin II is subserved by AT1 receptors.3 Angiotensin II (0.1-3 pM) produced concentration-dependent enhancement of both stimulationinduced (S-I) efflux of [3H]-noradrenaline and stimulation-evoked vasoconstrictor responses in isolated preparations of caudal artery from both SH and WKY rats, in which the noradrenergic transmitter stores had been labelled with [3H]-noradrenaline. The maximum enhancement of S-I efflux produced by angiotensin II (1 pM) was significantly greater in artery preparations from WKY rats than in preparations from SH rats, whereas the maximum enhancement of stimulation-evoked vasoconstrictor responses was greater in preparations from SH rats than in those from WKY rats. 4 In artery preparations from both WKY and SH rats, the AT1 angiotensin II receptor antagonist, losartan (0.01 and 0.1 pM), reduced or abolished the enhancement of both S-I efflux and vasoconstrictor responses by 1 pM angiotensin II. 5 The combination of 0.01 pM losartan and 0.1 IM angiotensin II enhanced both the S-I efflux and stimulation-evoked vasoconstrictor response in caudal artery preparations from WKY rats, whereas 0.1 UM angiotensin alone was ineffective. The AT2 receptor antagonist PD 123319 (0.01 and 0.1 pM) prevented the enhancement of both S-I efflux and stimulation-evoked vasoconstrictor responses by the combination of angiotensin II and losartan. 6 In contrast to findings in WKY preparations and those previously obtained for arteries from another normotensive strain (Sprague-Dawley), in artery preparations from SH rats there was no synergistic interaction between losartan and angiotensin II. Rather, combinations of 0.1 pM angiotensin II and PD 123319 (both 0.01 and 0.1 pM) enhanced S-I [3H]-noradrenaline efflux, whereas 0.1 pM angiotensin II alone was without effect. Moreover, losartan (0.1 pM) prevented the enhancement of S-I efflux by the combination of angiotensin II and PD 123319. 7 The present findings indicate that in the caudal artery of WKY and SH rats, and as previously found in Sprague-Dawley preparations, angiotensin II receptors similar to the ATIB subtype subserve enhancement of transmitter noradrenaline release. 8 As previously suggested for Sprague-Dawley caudal artery preparations, the synergistic prejunctional interaction of losartan and 0.1 pM angiotensin II in caudal artery preparations from WKY r...

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Section: Discussionsupporting

confidence: 80%

Section: Introductionmentioning

confidence: 59%

mentioning

confidence: 91%

Section: Introductionmentioning

confidence: 99%

mentioning

confidence: 99%

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Angiotensin II receptors involved in the enhancement of noradrenergic transmission in the caudal artery of the spontaneously hypertensive rat

Cox

Story

Ziogas

1996

British J Pharmacology

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Prejunctional modulation by angiotensins of noradrenaline release from sympathetic neurons in isolated rabbit aorta

Storgaard¹,

Nedergaard²

1997

Naunyn-Schmiedeberg's Arch Pharmacol

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The aims of the present work were to compare the modulating effect of angiotensins I, II, III, IV and (1-7) [AI, AII, AIII, AIV and A(1-7) respectively] on stimulation-evoked noradrenaline release from postganglionic sympathetic nerves in rabbit isolated aorta; to examine the influence of inhibiting the neuronal and extraneuronal uptake of noradrenaline on the modulating effect of AII and thirdly, to determine the role of angiotensin converting enzyme (ACE) in the modulating effects of AI and AII and the role of aminopeptidases A and M in the effects of AII and AIII. Rings of aorta were preloaded with (-)-3H-noradrenaline and then subjected to electrical field stimulation. Cumulative addition of AI (10(-8)-10(-6) M), AII (3 x 10(-11)-10(-8) M) and AIII (3 x 10(-10)-10(-6) M) enhanced the stimulation-evoked 3H-overflow up to 142, 165 and 188% respectively. The order of potency was AII > AIII > AI. AIV (10(-10)-10(-7) M) and A(1-7) (10(-10)-10(-7) M) caused no change. Single concentrations (10(-9)-10(-7) M) of AI, AII and AIII caused initial enhancement which subsequently decreased, i.e. development of tachyphylaxis. The effect of AII was independent of stimulation frequency at 1-10 Hz, but absent at 30 Hz. Cocaine (3 x 10(-5) M) plus corticosterone (4 x 10(-5) M) did not alter the enhancing effect of AII. CaNa2EDTA (3 x 10(-5) M) did not alter the enhancing effect of AI. Captopril (10(-6) and 10(-5) M) and lisinopril (10(-6) M) attenuated the enhancing effect of AI. Captopril and lisinopril (both 10(-6) and 10(-5) M) did not alter the enhancing effect of AII. Captopril (10(-7)-10(-4) M) and lisinopril (10(-7)-10(-4) M) themselves did not alter the stimulation-evoked 3H-overflow. Amastatin (10(-5) M) increased the enhancement seen with AIII (3 x 10(-11)-10(-9) M) but did not alter the enhancing effect of AII (10(-9)-10(-8) M). Amastatin (10(-9)-10(-5) M) had no effect on the stimulation-evoked 3H-overflow. It is concluded that AI, AII and AIII facilitate the stimulation-evoked 3H-noradrenaline release to various degrees (relative order of potency: AII > AIII > AI and of efficacy: AIII > AII > AI). The estimates may be compromised by the development of tachyphylaxis. The facilitation by AII was independent of the neuronal and extraneuronal uptake mechanisms. The action of AI is in part due to its conversion to AII. The effect of AIII was probably underestimated due to its degradation to AIV. AII is apparently not a substrate for aminopeptidase M.

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A comparison of AT 1 angiotensin II antagonists at pre- and postjunctional angiotensin II receptors of the rat tail artery

Pinheiro

Moura

Albino‐Teixeira

et al. 2002

Naunyn-Schmiedeberg's Archives of Pharmacology

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A comparison was made of the influence of candesartan, ZD7155, losartan and eprosartan on angiotensin II effects at pre- and postjunctional AT(1) receptors of the rat tail artery. To study the anti-angiotensin II effect at prejunctional receptors, the tissues were preincubated with [(3)H]noradrenaline and then superfused and electrically stimulated (1 Hz, 2 ms, 50 mA, during 5 min); to study the angiotensin II effect at postjunctional receptors, non-cumulative concentration-response curves to angiotensin II were determined in the absence and in the presence of the antagonist. p A(2) values were calculated for competitive antagonists and p D'(2) values for insurmountable antagonists. At the prejunctional level, losartan and eprosartan displayed competitive antagonism with p A(2) values of 6.50 and 8.08, respectively, whereas candesartan and ZD7155 displayed non-competitive antagonism with p D'(2) values of 8.71 and 7.98, respectively. At the postjunctional level, the four antagonists displayed the same kind of antagonism as prejunctionally with p A(2) values for losartan and eprosartan of 8.52 and 8.22, respectively, and p D'(2) values of 10.62 and 9.01, for candesartan and ZD7155, respectively. The ratios between post- and prejunctional potencies were: losartan 101, candesartan 81, ZD7155 11, and eprosartan 1.4. We conclude that, at least functionally, pre- and postjunctional angiotensin II AT(1) receptors are different and propose that the prejunctional receptors in this tissue belong to the AT(1B)-subtype.

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Evidence for the involvement of different receptor subtypes in the pre‐ and postjunctional actions of angiotensin II at rat sympathetic neuroeffector sites

Cited by 47 publications

References 25 publications

Angiotensin II receptors involved in the enhancement of noradrenergic transmission in the caudal artery of the spontaneously hypertensive rat

Angiotensin II receptors involved in the enhancement of noradrenergic transmission in the caudal artery of the spontaneously hypertensive rat

Prejunctional modulation by angiotensins of noradrenaline release from sympathetic neurons in isolated rabbit aorta

A comparison of AT 1 angiotensin II antagonists at pre- and postjunctional angiotensin II receptors of the rat tail artery

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