Histamine receptors in rabbit atria

Polanin, Alicia

January 1979

In order to characterize the types of histamine receptors (H₁ or H₂) in rabbit atria, isolated atrial preparations were exposed to selective histamine receptor agonists, alone and in the presence of selective histamine receptor antagonists. The rate of isolated right atria was increased by histamine (H₁ and H₂), 4-methylhistamine (H₂), and impromidine (H₂). 2-Pyridylethylamine (PEA, H₁) had very little effect on atrial rate. Cimetidine pretreatment (selective H₂ receptor blockade) competitively antagonized the positive chronotropic effects of histamine, 4-methylhistamine, and impromidine. Promethazine pretreatment (selective H₁ receptor blockade) competitively blocked the chronotropic effects of histamine, but had no effect on the responses to 4-methylhistamine or impromidine. The force of isolated left atria was increased by all four agonists. Cimetidine pretreatment competitively blocked the inotropic effects of histamine, 4-methylhistamine, and impromidine, and had no effect on the response to PEA. Promethazine pretreatment competitively blocked the inotropic responses to histamine and to PEA, and had no effect on the responses to 4-methylhistamine or impromidine. The phosphodiesterase inhibitor theophylline (3 x 10⁻⁴M) potentiated the inotropic but not the chronotropic effects of 4-methylhistamine. (1 x 10⁻⁴M , impromidine (1 x 10⁻⁸M) and PEA (1 x 10⁻⁴M) . Histamine (1 x 10⁻⁵M) exposure for 20 seconds did not alter the cyclic AMP levels of isolated rabbit right and left atria. We report that both types (H₁ and H₂) of histamine receptors are present in rabbit right and left atria. However, I cannot confirm reports (Hughes,1978) that both H₁ and H₂ histamine receptor agonists act through the generation of cyclic AMP. / Pharmaceutical Sciences, Faculty of / Graduate

Rabbits - physiology

Histamine

Receptors, drug

Effects of drugs on miniature end-plate currents at the mouse neuromuscular junction

Pennefather, Peter

January 1982

Digital averaging and analysis of miniature endplate currents (MEPCs) from mouse diaphragm was used to characterize the normal MEPC and its modification by a variety of drugs. Under normal conditions the decay of MEPCs showed consistent deviations from a simple exponential consisting in a progressive increase of rate constant, followed by a slow tail. Receptor blockade by d-tubocurarine (dTC), a-bungarotoxin, and other agents thought to occupy ACh-binding sites reduced MEPC amplitude, accelerated MEPC decay by about 30% (making it about equal to decay rate of channels opened by exogenous acetylcholine), and eliminated the early deviations from an exponential decay; dTC also abolished the late tail. Examination of the interaction of acetylcholinesterase (AChE) poisoning and receptor blockade on MEPC height and time course indicated that normally most quantal ACh is captured by receptors and, as predicted by theoretical consideration, a rather large degree of receptor blockade is necessary to reduce MEPC height. MEPC tails were exaggerated by AChE poisoning and exogenous ACh or carba-chol. The latter agents reduced MEPC height in a fashion inconsistent with blockade of ACh binding and concurrent modulation of the tail suggested an important role of desensitized receptors in tail generation. A number of other drug actions are also described quantitatively: (a) channel prolongation, typical of alcohols but also found with ketones and some amines; (b) 'channel plugging', typical of local anaesthetics but also found with many other agents, including long chain alcohols, and (c) an action to reduce MEPC size without reducing net response to exogenous agonist typical of volatile anaesthetics, associated with increase rather than decrease of ACh binding to receptor. Criteria for distinguishing different modes of modification of receptor function are discussed. / Medicine, Faculty of / Anesthesiology, Pharmacology and Therapeutics, Department of / Graduate

Neuromuscular transmission

Myoneural junction

Receptors, Drug

Neurotransmitter Agents

Neuromuscular Junction -- drug effects

Drug receptors