Effect of pirenzepine and gallamine on cardiac and pulmonary muscarinic receptors in the rabbit

Maclagan, Jennifer; Faulkner, David

doi:10.1111/j.1476-5381.1989.tb11979.x

Cited by 31 publications

(11 citation statements)

References 11 publications

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“…Higher doses of pirenzepine suppressed vagal regulation of myocardial activity probably due to atropine-like effects of cumulative doses. This explanation is in line with the finding that in a dose of 10 -6 mol/kg pirenzepine extends the spectrum of its blocking action with respect to differently located muscarinic receptors [11 ].…”

Section: R Es U Ltssupporting

confidence: 60%

Dynamics of vagal chronotropic effects during blockade of different types of muscarinic cholinergic receptors

Osadchii

Pokrovskii

1999

Bull Exp Biol Med

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Different changes in vagal chronotropic effects were observed in cats under blockade of various types of muscarinic cholinergic receptors. Burst stimulation of the vagus nerve caused synchronization of the vagal and cardiac rhythms, which was potentiated by M a and M 3 receptor antagonists and suppressed by the M 2 blocker gallamine. The components of the vagal chronotropic effect showed different sensitivity to selective M-cholinolytics.Key Words: muscarini cholinergic receptors; vagal chronotropic effect Heterogenous population of muscarinic cholinergic receptors includes at least 5 subtypes which are distinguished by their structure, location, and functional properties [7]. In the myocardium, M2receptors are the predominant type of receptors. They mediate the inhibitory effects of the vagus nerve (VN) stimulation. However, there is evidence that other types of cholinergic receptors are also implicated in the regulation of cardiac activity. For instance in rats and guinea pigs, the intracardial neurons contain RNAs encoding four types of muscarinic receptors (M1-M 4) [9]. Receptors of different types may play different functional roles. For instance, in dogs MI receptor blockade significantly weakened the vagal chronotropic effect (VCE), but did not affect the vagal influence on the myocardial conductivity and contractility [5,12].These findings can be used in the analysis of VCE mechanisms. Along with the inhibitory tonic component, the chronotropic effect contains a synchronizing component that controls cardiac rhythm under conditions of VN stimulation [13]. These components are probably associated with different muscarinic receptors. In this study we checked up this hypothesis. MATERIALS AND METHODSExperiments were carried out on 27 cats weighing 3-4 kg anesthetized with intraperitoneal Chloralose-NemDepartment Physiolo9y, Kuban Medical Academy, Krasnodar butai mixture (75:15 mg/kg) and 'artificially ventilated. The peripheral end of the right VN was stimulated with short 40 Hz trains of 3, 6, or 9 rectangular pulses of 0.2 msec duration and 5-6 thresholds' intensity. Amplified ECG was recorded by a unipolar probe inserted through the femoral vein into the right atrium. The following selective M-receptor antagonists were used: pirenzepine (M1), gallamine (M2), and 4-diphenylacetoxy-N-(2-chlorethyl)-piperidine (4-DAMP. M3) [6]. The drugs (0.002-0. 2 mg/kg ) were infused intravenously. The data were analyzed statistically by the method of direct differences [ 1 ].

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Section: R Es U Ltssupporting

confidence: 60%

Dynamics of vagal chronotropic effects during blockade of different types of muscarinic cholinergic receptors

Osadchii

Pokrovskii

1999

Bull Exp Biol Med

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“…In each of these examples, the receptors exerted an inhibitory control on cholinergic neurotransmission to airway smooth muscle. This autoreceptor mechanism appears to be lacking in the rabbit (Maclagan & Faulkner, 1989) and in asthmatic patients (Minette et al, 1988). Figure 2 shows the mechanisms that underlie the results presented in this paper and in previous work from this laboratory showing that M1 muscarinic receptors with a facilitatory function exist in the sympathetic nervous pathway in the guinea-pig lung (this paper) and M2 receptors exist in the parasympathetic nerves in this species (Fryer & Maclagan, 1984).…”

Section: Discussionmentioning

confidence: 60%

Identification of M₁ muscarinic receptors in pulmonary sympathetic nerves in the guinea‐pig by use of pirenzepine

Maclagan

Fryer

Faulkner

1989

British J Pharmacology

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1 The effect of pirenzepine, a muscarinic antagonist considered to be selective for M1 receptors, was studied on bronchoconstriction and bradycardia elicited by preganglionic stimulation of the parasympathetic vagal nerves and by i.v. injections of acetylcholine (ACh) in anaesthetized guinea- 4 Propranolol (1 mg kg-) increased control bronchoconstrictor responses elicited by ACh and vagal stimulation but did not alter the potency of pirenzepine for postjunctional receptors in heart or lung. However, pirenzepine-induced enhancement of vagally-induced bronchoconstriction was abolished by propranolol, suggesting that pirenzepine may be an antagonist for muscarinic receptors located in the sympathetic nerves innervating airway smooth muscle. 5These results confirm that bronchoconstrictor stimuli indirectly initiate activation of an opposing sympathetic reflex in the guinea-pig lung. This response is facilitated by muscarinic receptors located in the sympathetic nervous pathway. 6 The high potency of pirenzepine for the neuronal receptors in the sympathetic nerves suggests that these are M1 receptors. In contrast, the parasympathetic nerves innervating airway smooth muscle in this species contain M2 receptors which inhibit neurotransmission.

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“…Knowledge about cholinoceptors and especially muscarinic receptor subtypes in airway smooth muscle is available in many animal species such as guinea-pig, ox, dog, rat, rabbit and man, but not in mice (Fryer & Mclagan, 1984;Blaber et al, 1985;Van Koppen et al, 1985;Faulkner et al, 1986;Eglen & Whiting, 1986;O'Rourke et al, 1987;Madison et al, 1987;Beck et al, 1987;Bloom et al, 1987;Roffel et al, 1988;Ito & Yoshitomi, 1988;Maclagan & Faulkner, 1989 Values are mean ± s.e. mean (n = 15 for each antagonist; n = 5 for each concentration).…”

Section: Discussionmentioning

confidence: 99%

Functional characterization of muscarinic receptors in murine airways

Garssen

Loveren

Gierveld

et al. 1993

British J Pharmacology

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1 The effects of muscarinic receptor antagonists considered to be selective for Ml receptors (pirenzepine; PZ), M2 receptors (AFDX-1 16), and for M3 receptors (4-diphenyl acetoxy N-methylpiperidine (4-DAMP)) were used to investigate the existence of muscarinic receptor subtypes in murine airways. Atropine was used as a nonselective antagonist. The effects of these antagonists were studied upon tracheal contractions induced either by EFS (electric field stimulation) or by application of an exogenous cholinoceptor agonist (arecoline).2 The muscarinic receptor antagonists tested inhibited arecoline-induced tracheal contractions with the following rank order of potency: 4-DAMP = atropine> pirenzepine = AFDX-1 16. The rank order of potency of the muscarinic antagonists used in inhibiting EFS-induced tracheal contractions was: 4-DAMP = atropine> PZ> AFDX-1 16. The pA2 values for these antagonists were similar when compared to the pA2 values determined in guinea-pig and bovine airway smooth muscle. 3 In addition to in vitro studies, the effects of inhalation of the different muscarinic antagonists on lung function parameters in vivo were investigated. Inhalation of 4-DAMP induced a decrease in airway resistance and an increase in lung compliance. In contrast, inhalation of AFDX-116 induced an increase in airway resistance and almost no change in lung compliance. Apart from some minor effects of atropine on airway resistance, atropine, PZ, and pilocarpine failed to induce changes in lung mechanics as determined by in vivo lung function measurements. 4 The results provide evidence for the existence of M3 receptors on murine tracheae that are involved in the contraction of tracheal smooth muscle. This is in agreement with other animal species such as the guinea-pig and bovine. In vivo experiments also demonstrated that in the mouse, M3 receptors play an important role in bronchial smooth muscle contraction and thus in bronchoconstriction. Interestingly we have also demonstrated that M2 receptors can play a role in bronchodilatation. Inhalation of an M2 receptor antagonist induced an increase in airway resistance whereas inhalation of an M3 receptor antagonist induced a decrease in airway resistance. It is therefore likely that an M3/M2 receptor balance plays an important role in the regulation of airway function.

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Effect of pirenzepine and gallamine on cardiac and pulmonary muscarinic receptors in the rabbit

Cited by 31 publications

References 11 publications

Dynamics of vagal chronotropic effects during blockade of different types of muscarinic cholinergic receptors

Dynamics of vagal chronotropic effects during blockade of different types of muscarinic cholinergic receptors

Identification of M₁ muscarinic receptors in pulmonary sympathetic nerves in the guinea‐pig by use of pirenzepine

Functional characterization of muscarinic receptors in murine airways

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Effect of pirenzepine and gallamine on cardiac and pulmonary muscarinic receptors in the rabbit

Cited by 31 publications

References 11 publications

Dynamics of vagal chronotropic effects during blockade of different types of muscarinic cholinergic receptors

Dynamics of vagal chronotropic effects during blockade of different types of muscarinic cholinergic receptors

Identification of M1 muscarinic receptors in pulmonary sympathetic nerves in the guinea‐pig by use of pirenzepine

Functional characterization of muscarinic receptors in murine airways

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Identification of M₁ muscarinic receptors in pulmonary sympathetic nerves in the guinea‐pig by use of pirenzepine