Rudolf Hammer scite author profile

Some antagonists exhibit tissue selectivity in their pharmacological antagonism of muscarinic responses. However, the affinity constants for equilibrium binding of classical antagonists to muscarinic receptors in subcellular preparations have shown only small variations in different peripheral tissues and regions of the brain. The binding curves do not deviate significantly from the simple Langmuir isotherm, indicating apparent homogeneity of the receptor population in any given region. In contrast, heterogeneity has been detected by agonist binding studies but this may arise from different environmental or coupling restraints on the agonist-induced conformational change and cannot be taken as evidence for different receptor subtypes. We report here binding studies using a new anti-muscarinic drug, pirenzepine, in which we found heterogeneity of binding that correlates well with the pharmacological activity.

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Muscarinic receptor subtypes: M1 and M2 biochemical and functional characterization

Hammer

1982

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Tiotropium (SPIRIVA™): Mechanistical considerations and clinical profile in obstructive lung disease

et al. 1999

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Binding profile of a novel cardioselective muscarine receptor antagonist, AF-DX 116, to membranes of peripheral tissues and brain in the rat

et al. 1986

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Ba 679 BR, A novel long-acting anticholinergic bronchodilator

et al. 1993

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Rudolf Hammer

Pirenzepine distinguishes between different subclasses of muscarinic receptors

Muscarinic receptor subtypes: M1 and M2 biochemical and functional characterization

Tiotropium (SPIRIVA™): Mechanistical considerations and clinical profile in obstructive lung disease

Binding profile of a novel cardioselective muscarine receptor antagonist, AF-DX 116, to membranes of peripheral tissues and brain in the rat

Ba 679 BR, A novel long-acting anticholinergic bronchodilator

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