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Methoctramine selectively blocks cardiac muscarinic M2 receptors in vivo (1988)

Wess, Jürgen ; Angel, Piero ; Melchiorre, Carlo ; [et al.]

Springer

Naunyn-Schmiedeberg's archives of pharmacology 338 (1988), S. 246-249

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ISSN: 1432-1912

Keywords: Methoctramine ; Polymethylene tetraamines ; Cardioselectivity ; M1/M2 receptors ; Muscarinic receptor subtypes

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The antimuscarinic effects of methoctramine (N, N′- bis[6-[(2-methoxybenzyl)amino]hexyl]-1,8-octanediamine tetrahydrochloride), a polymethylene tetraamine endowed with high cardioselectivity in vitro, were assessed in two in vivo preparations. Methoctramine (300 μg/kg i.v.) strongly inhibited the methacholine- and muscarine-induced bradycardia in the anaesthetized and pithed rat, respectively. The same dose of methoctramine did not significantly affect the depressor action of methacholine in the anaesthetized rat mediated by vascular M2 receptors. Furthermore, even high doses of methoctramine (up to 1 mg/kg i. v.) did not reduce the ganglionic M1 receptor-mediated tachycardia and pressor response to muscarine or McN-A-343 in the pithed rat. These data suggest that methoctramine while showing high affinity for cardiac M2α receptors has rather low affinity for ganglionic M1 and vascular M2 receptors. This in vivo study thus provides further evidence to support the view that methoctramine is a potent and highly selective antagonist of cardiac M2α receptors.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00173395

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Sila-Pharmaka, 371) Darstellung und Eigenschaften der Enantiomere der Antimuskarinika Sila-Procyclidin und Sila-Tricyclamol-iodid: Optisch aktive Silanole mit Silicium als Chiralitätszentrum2) (1987)

Tacke, Reinhold ; Linoh, Haryanto ; Ernst, Ludger ; [et al.]

Weinheim : Wiley-Blackwell

Berichte der deutschen chemischen Gesellschaft 120 (1987), S. 1229-1237

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ISSN: 0009-2940

Keywords: Chemistry ; Inorganic Chemistry

Source: Wiley InterScience Backfile Collection 1832-2000

Topics: Chemistry and Pharmacology

Description / Table of Contents: Sila-Pharmaca, 371). - Preparation and Properties of tbe Enantiomers of the Antimuscarinic Agents Sila-Procyclidine and Sila-Tricyclamol Iodide: optically Active Silanols with Silicon as the Centre of Chirality2)The enantiomers of sila-procyclidine (R)-1b and (S)-1b [ 〉 97% ee (NMR), 99.7% ee (DSC)] were obtained by resolution with L-(+)- and D-(-)-tartaric acid, respectively. Starting from (R)-1b and (S)-1b, the hydrochlorides (R)-2b and (S)-2b were prepared and the enantiomers of sila-tricyclamol iodide (R)-3b and (S)-3b [ 〉 96% ee (NMR)] were synthesized by reaction with CH3I. The optically active silanols show configurational stability in the crystalline state and in inert solvents, whereas they racemize in aqueous solution (3b faster than 1b). By analogy with the stereoselectivity of antimuscarinic action of the enantiomers of the carbon analogues procyclidine (1a) and tricyclamol iodide (3a), the (R) enantiomers of 1b and 3b show a greater affinity for the ileal M2β and atrial M2α muscarinic receptors of the guinea pig than the corresponding (S) antipodes. All silicon compounds exhibit a greater antimuscarinic potency than their carbon analogues, whereas the stereoselectivity of action is more pronounced for the carbon compounds. The differences in affinity for (R)-1b and (S)-1b for ileal and atrial muscarinic receptors confirm the present concept of heterogeneity in muscarinic M2 receptors (M2α: atrial type; M2β: ileal type).

Notes: Durch Racematspaltung mit L-(+)- bzw. D-(-)-Weinsäure wurden die Enantiomere des Sila-Procyclidins (R)-1b und (S)-1b erhalten [〉 97% ee (NMR), 99.7% ee (DSC)]. Daraus wurden die Hydrochloride (R)-2b und (S)-2b und durch Umsetzung mit CH3I die Enantiomere des Sila-Tricyclamol-iodids (R)-3b und (S)-3b [ 〉 96% ee (NMR)] hergestellt. Die optisch aktiven Silanole sind in kristalliner Form und in inerten Lösungsmitteln konfigurationsstabil, während sie in wässeriger Lösung racemisieren (3b schneller als 1b). In Analogie zur Stereoselektivität der antimuskarinischen Wirkung der Enantiomere der Kohlenstoff-Analoga Procyclidin (1a) und Tricyclamol-iodid (3a) besitzen die (R)-Enantiomere von 1b und 3b eine größere Affinität zu den ilealen M2β- und atrialen M2α- Muskarinrezeptoren des Meerschweinchens als die (S)-Antipoden. Alle Silicium-Verbindungen sind stärker antimuskarinisch wirksam als ihre Kohlenstoff-Analoga, deren Stereoselektivität jedoch stärker ausgeprägt ist. Die Unterschiede in der Affinität von (R)-1b und (S)-1b zu den ilealen und atrialen Muskarinrezeptoren bestätigen das Konzept der Heterogenität muskarinischer M2-Rezeptoren (M2α: atrialer Typ; M2β: ilealer Typ).

Additional Material: 2 Ill.