Subtypes of muscarinic receptor on cholinergic nerves and atrial cells of chicken and guinea‐pig hearts

Jeck, D.; Lindmar, R.; Löffelholz, K.; Wänke, Michaela

doi:10.1111/j.1476-5381.1988.tb11442.x

Cited by 40 publications

(14 citation statements)

References 11 publications

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“…Presynaptie M 1 -receptors have also been found in ehieken heart (Jeck et al, 1988), different guinea-pig and rat brain areas (Belleroehe and Gardiner, 1985;Marehi et al, 1986;Williams and Constanti, 1988) as weil as in guinea-pig and rat small intestine (Mieheletti et al, 1988;Sehwörer and K.ilbinger, 1988). However, it remains to be elueidated whether all these presynaptie musearlnie reeeptors are pharmacologieally identieal or whether they belang to different M 1 -reeeptor subclasses.…”

Section: Discussionmentioning

confidence: 99%

Presynaptic muscarinic receptors mediating inhibition of neurogenic contractions in rabbit vas deferens are of the ganglionic M1-type

Eltze

Gmelin

Wess

et al. 1988

European Journal of Pharmacology

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The present study was designed to further eharaeterize the presynaptie musearlnie M 1 -reeeptor responsible for the inhibition of neuragenie eontraetions in the isolated rabbit vas deferens. Eleetrically induced twiteh eontraetions of this preparation were inhibited by the M 1 -agonist, MeN-A-343, and by some of its analogs: 4-ehloro-phenyl derivative> MeN-A-343 > trans-olefinie analog> cis-olefinie analog. The same rank order of potency was obserVed for these agonists to raise the blood pressure of pithed rats by stimulation of M 1 -receptors in sympathetie ganglia. A highly signifieant eorrelation was found between the antimusearinie potencies of atropine, pirenzepine and a series of 9 antagonists strueturally related to the ganglionie M 1 p-receptor selective compounds, hexocyclium and hexahydro-difenidol, to antagonize the MeN-A-343-indueed inhibition of twitch eontraetions in rabbit vas deferens or the musearine-indueed depolarization in rat isolated superior eerVieal ganglia. I t is suggested that the presynaptie musearlnie receptor that mediates inhibition of neuragenie contraetions in rabbit vas deferens is of the ganglionic M 1 p-type.Musearlnie receptor subtypes; Vas deferens (rabbit); Pithed rat; Ganglia (rat); Musearlnie aeetyleholine receptor agonists; Musearlnie aeetyleholine receptor antagonists; MeN-A-343 analogs

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Section: Discussionmentioning

confidence: 99%

Presynaptic muscarinic receptors mediating inhibition of neurogenic contractions in rabbit vas deferens are of the ganglionic M1-type

Eltze

Gmelin

Wess

et al. 1988

European Journal of Pharmacology

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“…Such receptors have previously been described in the cardiac nerves in the rat (Wetzel & Brown, 1985) and in the guinea-pig (Jeck et al, 1988). Blockade of these receptors by gallamine would increase transmitter output from the vagus nerves and increase the concentration of antagonist required to inhibit vagallyinduced bradycardia.…”

Section: Discussionmentioning

confidence: 99%

“…At present, the guinea-pig is the only species in which M2 receptors have been demonstrated in both pulmonary (Fryer & Maclagan, 1984) and cardiac (Jeck et al, 1988) parasympathetic nerves.…”

Section: Discussionmentioning

confidence: 99%

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

Maclagan

Faulkner

1989

British J Pharmacology

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1 The effect of muscarinic antagonists considered to be selective for M1 receptors (pirenzepine) and for M2 receptors (gallamine) were studied on bronchoconstriction and bradycardia elicited by stimulation of the vagal nerves and by i.v. acetylcholine (ACh) in anaesthetized rabbits. 2 Pirenzepine was equipotent as an antagonist of ACh-induced responses at postjunctional muscarinic receptors in the heart, lung and blood vessels, whereas gallamine was at least ten times less potent at pulmonary and vascular muscarinic receptors. Thus, gallamine never caused complete inhibition of bronchoconstrictor or hypotensive responses to i.v. ACh, whereas doses of pirenzepine in excess of 1 pmol kg1-abolished all muscarinic responses. 3 In the lung, both antagonists inhibited bronchoconstriction caused by vagal stimulation and ACh-induced bronchoconstriction to the same extent (pirenzepine, mean ED50 65 + 22 and 130 + 28nmolkg-1 respectively; gallamine, ED50> 10,OOOnmolkg-1 for both responses).Enhancement of vagally-induced bronchoconstriction was never observed. 4 In the heart, however, both pirenzepine and gallamine were ten times less potent as antagonists of vagally-induced bradycardia than of ACh-induced bradycardia. This differential blockade was unaltered by propranolol (1 mg kg-1) pretreatment. 5 It is concluded that there is no evidence for M1 or M2 muscarinic receptors in the pulmonary innervation of the rabbit and the potency of the antagonists in abolishing vagally-induced bronchoconstriction was consistent with blockade of M3 muscarinic receptors on airway smooth muscle. 6 The results suggest that M2 muscarinic receptors may exert an inhibitory effect on transmission in the parasympathetic nerves innervating the heart in the rabbit. Blockade of such neuronal receptors would increase transmitter output to the atrial cells and explain the low potency of both antagonists in abolishing vagally-induced bradycardia in the rabbit.

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“…The high affinity of chick cardiac receptors for pirenzepine has been observed repeatedly (Brown et al, 1985;Lindmar & Loffelholz, 1987;Jeck et al, 1988;Choo et al, 1988;Lazareno et al, 1990;Tietje & Nathanson, 1991), although low affinity was found by Sorota et al (1986). (2) The M2-like sites in chick heart have a slightly lower Kd for NMS than the M4-like population, while in mammalian tissues, the affinity of M4 receptors for NMS is higher than that of M2 receptors (Waelbroeck et al, 1990;Lazareno et al, 1990).…”

Section: Effect Of Alcuronium On the Dissociation Of [3h]-nmsmentioning

confidence: 93%

“…They appear similar to the Ml subtype because of their high affinity for pirenzepine (Brown et al, 1985;Lindmar & Loffelholz, 1987;Jeck et al, 1988), but the pattern of affinities of other ' Author for correspondence.…”

Section: Introductionmentioning

confidence: 99%

Two populations of muscarinic binding sites in the chick heart distinguished by affinities for ligands and selective inactivation

Jakubík

Tuček

1994

British J Pharmacology

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Both populations have high affinities for pirenzepine, but the affinity of the former (major) population is lower (pKi = 7.99) than that of the latter (minor) population (pKi = 10.14). 2 Since it has been shown earlier that two mRNAs for muscarinic receptors are expressed in the chick heart, one of them close to the genetically defined m2 and the other to the m4 subtype, we propose that the major population of binding sites with high affinities for AF-DX1 16

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Subtypes of muscarinic receptor on cholinergic nerves and atrial cells of chicken and guinea‐pig hearts

Cited by 40 publications

References 11 publications

Presynaptic muscarinic receptors mediating inhibition of neurogenic contractions in rabbit vas deferens are of the ganglionic M1-type

Presynaptic muscarinic receptors mediating inhibition of neurogenic contractions in rabbit vas deferens are of the ganglionic M1-type

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

Two populations of muscarinic binding sites in the chick heart distinguished by affinities for ligands and selective inactivation

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