α<sub>2</sub>‐Adrenoceptor agonists enhance responses to certain other vasoconstrictor agonists in the rat tail artery

Xiao, Xiao-Hui; Rand, M. J.

doi:10.1111/j.1476-5381.1989.tb11851.x

Cited by 37 publications

(21 citation statements)

References 28 publications

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“…It has previously been suggested that, in certain vascular beds, simultaneous activation of l-and M2-adrenoceptors is required before the responses to a2-adrenoceptor stimulation are observed, e.g. in the rabbit saphenous artery (Dunn et al, 1991b) and rat tail artery (Xiao & Rand, 1989). It is likely, therefore, that such interactions may involve complex facilitatory interactions between alr-and M2-adrenoceptor-induced calcium ion channel activation and membrane potential changes.…”

Section: Discussionmentioning

confidence: 99%

Influences of the endothelium and hypoxia on α₁‐ and α₂‐adrenoceptor‐mediated responses in the rabbit isolated pulmonary artery

MacLean

McCulloch

McGrath

1993

British J Pharmacology

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1 The effects of the inhibitor of nitric oxide synthase, N'0-nitro-L-arginine methylester (L-NAME, i0' M), mechanical disruption of the endothelium and hypoxia on contraction to noradrenaline (al-and x2-adrenoceptor agonist), phenylephrine (a,-adrenoceptor agonist) and UK 14304 (@2-adrenoceptor agonist) were compared in the rabbit isolated pulmonary artery. The effects of the selective antagonists rauwolscine (10-6 M, M2-adrenoceptors) and prazosin (10-' M, ax-adrenoceptors) on the contractions to noradrenaline before and after exposure to L-NAME were also assessed. 2 Noradrenaline, phenylephrine and UK 14304 all produced concentration-dependent increases in vascular tone. The responses to noradrenaline were sensitive to both rauwolscine and prazosin (effect of prazosin > > rauwolscine). L-NAME increased the potency of both noradrenaline and UK 14304, and also the maximum tension achieved. It had no effect on the responses to phenylephrine. After L-NAME, contractions to noradrenaline, although still sensitivie to both rauwolscine and prazosin, were now more sensitive to inhibition by rauwolscine. 3 Endothelium removal augmented the potency and maximum contractions to noradrenaline, phenylephrine and UK 14304. 4 Hypoxia decreased both the potency of phenylephrine and its maximum contractile response, but increased the maximum response to noradrenaline without effecting responses to UK 14304. 5 In conclusion, in the rabbit pulmonary artery, augmentation of contractile responses to noradrenaline by L-NAME involves a potentiation of a2-adrenoceptor-mediated contraction probably through an effect on the synthesis of endothelium-derived nitric oxide. Experimental hypoxia had differential effects on all three agonists and did not mimic the effect of nitric oxide synthase inhibition.

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Section: Discussionmentioning

confidence: 99%

Influences of the endothelium and hypoxia on α₁‐ and α₂‐adrenoceptor‐mediated responses in the rabbit isolated pulmonary artery

MacLean

McCulloch

McGrath

1993

British J Pharmacology

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“…The 5-HT receptor is of the 5-HT 2 receptor class 21 (supported by inhibition of 5-HT-induced contraction by the 5-HT 2 receptor antagonist LY53857), the ET-1 receptor is an ET A receptor, 22 and the ␣-adrenergic receptor is a mixture of ␣ 1 -and ␣ 2 -adrenergic receptors. 23,24 All 3 classes of receptors activate similar, classic signaling pathways (plasma membrane calcium channels and phospholipase C), and all receptors have recently been identified as being able to activate the Erk MAPK pathway in vascular smooth muscle. Several investigators have demonstrated that Erk MAPK can phosphorylate caldesmon and, in doing so, release the calmodulin-mediated inhibition of actinomyosin ATPase and thereby promote smooth muscle contraction.…”

Section: Discussionmentioning

confidence: 99%

5-Hydroxytryptamine–Induced Potentiation of Endothelin-1– and Norepinephrine-Induced Contraction Is Mitogen-Activated Protein Kinase Pathway Dependent

Watts

2000

Hypertension

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Abstract-5-Hydroxytryptamine (5-HT)-induced arterial contraction depends on activation of the tyrosine kinasedependent extracellular signal-regulated mitogen-activated protein kinase (Erk MAPK) pathway. The importance of 5-HT in the control of peripheral resistance has been questioned because circulating free levels of 5-HT are low (in the nanomolar range). We tested the hypothesis that physiologically relevant concentrations of 5-HT potentiate arterial contraction in response to agonists proved to have importance in blood pressure maintenance (norepinephrine [NE] and endothelin-1 [ET-1]) in a tyrosine kinase-and an Erk MAPK-dependent manner. Strips of endothelium-denuded rat tail artery were used for the measurement of isometric force. The general tyrosine kinase inhibitor genistein (5 mol/L) and the inhibitor of MAPK/Erk kinase activation PD098059 (10 mol/L) shifted concentration-response curves to 5-HT (1ϫ10 Ϫ9 to 3ϫ10 Ϫ4 mol/L) rightward but did not shift concentration-response curves to NE or ET-1. In separate experiments, 5-HT (10 nmol/L) potentiated contraction in response to NE (20 nmol/L) by Ϸ200% to 300% and to ET-1 (0.3 and 1 nmol/L) by 640% and 180%, respectively. Genistein and PD098059 significantly (66% to 100%) reduced 5-HT-induced potentiation of both NE (20 nmol/L)-and ET-1 (0.3 and 1 nmol/L)-induced contraction. Thus, these data support the ability of low physiological concentrations of 5-HT to amplify arterial responses to hormones with bona fide effects on blood pressure in the novel manner of depending on a tyrosine kinase/Erk MAPK pathway. Although these findings were generated in large arteries, we speculate that they may be applicable to vascular functioning in the deoxycorticosterone acetate salt model of hypertension in which all 3 hormones, 5-HT, NE, and ET-1, have been implicated as causal factors. Key Words: norepinephrine Ⅲ endothelin Ⅲ protein kinases Ⅲ arteries Ⅲ hormones S ince its discovery in serum in 1948, 1 5-hydroxytryptamine (5-HT [serotonin]) has been of interest to the cardiovascular researcher. 5-HT has been implicated in numerous cardiovascular diseases; vascular reactivity to 5-HT is increased in arteries from animals with different forms of hypertension 2 and atherosclerosis. 3 However, it has been argued that 5-HT plays an insignificant role in the physiological control of blood vessel tone because uptake of 5-HT by platelets, adrenergic nerves, or both causes circulating levels of 5-HT to be low (estimated to be 15 to 120 nmol/L 4 ) and out of a range that can directly cause constriction. One manner by which physiological concentrations of 5-HT may exert an effect on vascular tone is through the potentiation of vascular contraction in response to other vasoactive substances.5-HT-stimulated potentiation of agonist-induced contraction has classically been studied in the tail artery of the rat. [5][6][7] Norepinephrine (NE) was one of the first agonists established to be potentiated by 5-HT. The list of hormones of which contraction can be potentiated by 5-HT has grow...

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“…Activation of the postjunctional a2-adrenoceptors not only causes a direct contractile action but also en hances the responses to various contractile agents (5,18,19). Therefore, it is likely that, like KT-611, the drugs which have an antago nistic action to both postjunctional a 1 and a2 adrenoceptors may become more beneficial for the control of adrenergic responses in blood vessels and other tissues.…”

Section: Discussionmentioning

confidence: 99%

Pharmacological profile of the novel .ALPHA.-adrenoceptor antagonist KT-611(naftopidil).

Muramatsu¹,

Yamanaka²,

Kigoshi³

1991

Jpn.J.Pharmacol

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ABSTRACT-The pharmacological profile of a new alpha-adrenoceptor antagonist, , was studied in vitro. In the dog mesenteric and carotid arteries and in the rabbit, guinea pig and rat thoracic aortae, KT-611 competitively inhibited a 1-adrenoceptor-mediated contractions induced by noradrenaline with pA2 values ranging from 6.73 to 8.15. KT-611 also inhibited the postjunctional a2-adrenoceptor mediated contractions in the dog saphenous vein (pA2 = 6.77) or dog basilar artery. However, the responses mediated through prejunctional a2-adrenoceptors (rat vas deferens), /3-adrenoceptors (rat atria), muscarinic receptors (guinea pig ileum) and 5 HT2 receptors (dog mesenteric artery) were little affected by KT-611. KT-611 also in hibited the sympathetic adrenergic contraction evoked by electrical transmural stimu lation in the dog mesenteric artery, and the inhibition was not relieved upon repetitive washing for 1 hour with the drug-free solution. 3H-prazosin and 3H-clonidine binding to the rat cortex membranes was inhibited by KT-611 with pK; values of 7.69 and 5.75, respectively. These results suggest that KT-611 is an a 1-adrenoceptor antago nist with a weak antagonistic activity to postjunctional a2-adrenoceptors.

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α₂‐Adrenoceptor agonists enhance responses to certain other vasoconstrictor agonists in the rat tail artery

Cited by 37 publications

References 28 publications

Influences of the endothelium and hypoxia on α₁‐ and α₂‐adrenoceptor‐mediated responses in the rabbit isolated pulmonary artery

Influences of the endothelium and hypoxia on α₁‐ and α₂‐adrenoceptor‐mediated responses in the rabbit isolated pulmonary artery

5-Hydroxytryptamine–Induced Potentiation of Endothelin-1– and Norepinephrine-Induced Contraction Is Mitogen-Activated Protein Kinase Pathway Dependent

Pharmacological profile of the novel .ALPHA.-adrenoceptor antagonist KT-611(naftopidil).

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α2‐Adrenoceptor agonists enhance responses to certain other vasoconstrictor agonists in the rat tail artery

Cited by 37 publications

References 28 publications

Influences of the endothelium and hypoxia on α1‐ and α2‐adrenoceptor‐mediated responses in the rabbit isolated pulmonary artery

Influences of the endothelium and hypoxia on α1‐ and α2‐adrenoceptor‐mediated responses in the rabbit isolated pulmonary artery

5-Hydroxytryptamine–Induced Potentiation of Endothelin-1– and Norepinephrine-Induced Contraction Is Mitogen-Activated Protein Kinase Pathway Dependent

Pharmacological profile of the novel .ALPHA.-adrenoceptor antagonist KT-611(naftopidil).

Contact Info

Product

Resources

About

α₂‐Adrenoceptor agonists enhance responses to certain other vasoconstrictor agonists in the rat tail artery

Influences of the endothelium and hypoxia on α₁‐ and α₂‐adrenoceptor‐mediated responses in the rabbit isolated pulmonary artery

Influences of the endothelium and hypoxia on α₁‐ and α₂‐adrenoceptor‐mediated responses in the rabbit isolated pulmonary artery