Characterization of prejunctional muscarinic autoreceptors in the guinea‐pig trachea

1 The effects of ten muscarinic antagonists on electrically evoked [3H]‐acetylcholine release and muscle contraction were compared in an epithelium‐free preparation of the guinea‐pig trachea that had been preincubated with [3H]‐choline. 2 The M3‐selective antagonists UH‐AH 37, 4‐diphenyl‐acetoxy‐N‐p...

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Published inBritish journal of pharmacology Vol. 103; no. 3; pp. 1757 - 1763
Main Authors Kilbinger, H., Schneider, R., Siefken, H., Wolf, D., D'Agostino, G.
Format Journal Article
LanguageEnglish
Published Oxford, UK Blackwell Publishing Ltd 01.07.1991
Nature Publishing
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Abstract 1 The effects of ten muscarinic antagonists on electrically evoked [3H]‐acetylcholine release and muscle contraction were compared in an epithelium‐free preparation of the guinea‐pig trachea that had been preincubated with [3H]‐choline. 2 The M3‐selective antagonists UH‐AH 37, 4‐diphenyl‐acetoxy‐N‐piperidine methobromide and para‐fluorohexahydrosiladiphenidol were more potent in reducing the contractile response than in facilitating the evoked [3H]‐acetylcholine release. Hexahydrosiladiphenidol did not discriminate between pre‐ and postjunctional effects. The rank order of the postjunctional potencies of the ten antagonists as well as the postjunctional pA2 values obtained for hexahydrosiladiphenidol (7.95) and AQ‐RA 741 (7.08) identified the muscular receptor as an M3 subtype. 3 The M2‐selective antagonists methoctramine, AF‐DX 116 and AQ‐RA 741 were more potent in facilitating the evoked [3H]‐acetylcholine release than in inhibiting the contractile response. The increase in release by low concentrations of methoctramine, AF‐DX 116 and AQ‐RA 741 was paralleled by an enhancement of the stimulation‐evoked contractions. 4 Comparison of the pre‐ and postjunctional potencies of the M1‐, M2‐ and M3‐selective antagonists suggests that autoinhibition of acetylcholine release is mediated via an ‘M2‐like’ receptor which differs from the cardiac type M2 receptor in its relatively high affinity for hexahydrosiladiphenidol.
AbstractList 1. The effects of ten muscarinic antagonists on electrically evoked [3H]-acetylcholine release and muscle contraction were compared in an epithelium-free preparation of the guinea-pig trachea that had been preincubated with [3H]-choline. 2. The M3-selective antagonists UH-AH 37, 4-diphenyl-acetoxy-N-piperidine methobromide and para-fluorohexahydrosiladiphenidol were more potent in reducing the contractile response than in facilitating the evoked [3H]-acetylcholine release. Hexahydrosiladiphenidol did not discriminate between pre- and postjunctional effects. The rank order of the postjunctional potencies of the ten antagonists as well as the postjunctional pA2 values obtained for hexahydrosiladiphenidol (7.95) and AQ-RA (7.08) identified the muscular receptor as an M3 subtype. 3. The M2-selective antagonists methoctramine, AF-DX 116 and AQ-RA 741 were more potent in facilitating the evoked [3H]-acetylcholine release than in inhibiting the contractile response. The increase in release by low concentrations of methoctramine, AF-DX 116 and AQ-RA 741 was paralleled by an enhancement of the stimulation-evoked contractions. 4. Comparison of the pre- and postjunctional potencies of the M1-, M2- and M3-selective antagonists suggests that autoinhibition of acetylcholine release is mediated via an 'M2-like' receptor which differs from the cardiac type M2 receptor in its relatively high affinity for hexahydrosiladiphenidol.
1 The effects of ten muscarinic antagonists on electrically evoked [3H]‐acetylcholine release and muscle contraction were compared in an epithelium‐free preparation of the guinea‐pig trachea that had been preincubated with [3H]‐choline. 2 The M3‐selective antagonists UH‐AH 37, 4‐diphenyl‐acetoxy‐N‐piperidine methobromide and para‐fluorohexahydrosiladiphenidol were more potent in reducing the contractile response than in facilitating the evoked [3H]‐acetylcholine release. Hexahydrosiladiphenidol did not discriminate between pre‐ and postjunctional effects. The rank order of the postjunctional potencies of the ten antagonists as well as the postjunctional pA2 values obtained for hexahydrosiladiphenidol (7.95) and AQ‐RA 741 (7.08) identified the muscular receptor as an M3 subtype. 3 The M2‐selective antagonists methoctramine, AF‐DX 116 and AQ‐RA 741 were more potent in facilitating the evoked [3H]‐acetylcholine release than in inhibiting the contractile response. The increase in release by low concentrations of methoctramine, AF‐DX 116 and AQ‐RA 741 was paralleled by an enhancement of the stimulation‐evoked contractions. 4 Comparison of the pre‐ and postjunctional potencies of the M1‐, M2‐ and M3‐selective antagonists suggests that autoinhibition of acetylcholine release is mediated via an ‘M2‐like’ receptor which differs from the cardiac type M2 receptor in its relatively high affinity for hexahydrosiladiphenidol.
Author Schneider, R.
Kilbinger, H.
Siefken, H.
D'Agostino, G.
Wolf, D.
AuthorAffiliation Pharmakologisches Institut, Universität Mainz, F.R.G
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Issue 3
Keywords Rodentia
Autoreceptor
Respiratory system
In vitro
Characterization
Vertebrata
Mammalia
Guinea pig
Animal
Acetylcholine
Muscarinic receptor
Trachea
Release
Language English
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Snippet 1 The effects of ten muscarinic antagonists on electrically evoked [3H]‐acetylcholine release and muscle contraction were compared in an epithelium‐free...
1. The effects of ten muscarinic antagonists on electrically evoked [3H]-acetylcholine release and muscle contraction were compared in an epithelium-free...
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SubjectTerms Acetylcholine - isolation & purification
Acetylcholine - metabolism
acetylcholine release
Air breathing
Animals
Biological and medical sciences
Choline - isolation & purification
Choline - metabolism
Electric Stimulation
Fundamental and applied biological sciences. Psychology
Guinea Pigs
In Vitro Techniques
M2 receptors
M3 receptors
muscarinic autoreceptors
Muscle Contraction - drug effects
Muscle, Smooth - drug effects
Muscle, Smooth - metabolism
Parasympatholytics - pharmacology
Receptors, Muscarinic - drug effects
Respiratory system: anatomy, metabolism, gas exchange, ventilatory mechanics, respiratory hemodynamics
Trachea
Trachea - drug effects
Trachea - metabolism
Vertebrates: respiratory system
Title Characterization of prejunctional muscarinic autoreceptors in the guinea‐pig trachea
URI https://onlinelibrary.wiley.com/doi/abs/10.1111%2Fj.1476-5381.1991.tb09859.x
https://www.ncbi.nlm.nih.gov/pubmed/1933138
https://search.proquest.com/docview/72168861
https://pubmed.ncbi.nlm.nih.gov/PMC1907820
Volume 103
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