Neural and myogenic effects of cyclooxygenase products on canine bronchial smooth muscle

In canine bronchi bathed in 10(-6) M indomethacin (IDM), prostaglandin (PG) E2 inhibited electrical field stimulation (EFS)- and acetylcholine (ACh)-mediated contractions and excitatory junction potentials (EJP) in a concentration-dependent manner without altering the resting membrane potential. EFS...

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Bibliographic Details
Published inThe American journal of physiology Vol. 268; no. 1 Pt 1; p. L47
Main Authors Abela, A P, Daniel, E E
Format Journal Article
LanguageEnglish
Published United States 01.01.1995
Subjects
Animals
Bronchi - drug effects
Bronchi - innervation
Bronchi - physiology
Dinoprostone - pharmacology
Dogs
Electric Stimulation
Electrophysiology
Gap Junctions - physiology
Muscle Contraction - physiology
Muscle, Smooth - drug effects
Muscle, Smooth - innervation
Muscle, Smooth - physiology
Nervous System Physiological Phenomena
Prostaglandin-Endoperoxide Synthases - metabolism
Prostaglandins - pharmacology
Thromboxane A2 - pharmacology
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Summary:In canine bronchi bathed in 10(-6) M indomethacin (IDM), prostaglandin (PG) E2 inhibited electrical field stimulation (EFS)- and acetylcholine (ACh)-mediated contractions and excitatory junction potentials (EJP) in a concentration-dependent manner without altering the resting membrane potential. EFS-induced EJPs were abolished at 10(-7) M PGE2, which shifted responses to ACh 10-fold rightward. Thus PGE2 predominantly inhibited the release of ACh and secondarily decreased smooth muscle response to ACh. U-46619, an analogue of thromboxane A2 (TxA2), initiated tetrodotoxin- and atropine-insensitive contractions in a concentration-dependent manner. U-46619 (10(-9) M) did not alter significantly EFS- or ACh-stimulated contractions and potentiated EFS amplitude of EJPs without depolarizing muscle cells. Either prejunctional activation of ACh release by TxA2 or postjunctional potentiation of the response to ACh can explain these findings. U-46619 (> or = 10(-8) M) depolarized the membrane potential, initiating oscillations accompanied by a large contraction. Addition of 10(-8) M nitrendipine, but not tetraethylammonium (25 mM), blocked the oscillations selectively. Other prostanoids (PGD2, PGI2, and PGF2 alpha) had no significant effects on canine bronchi. In the absence of IDM, PGE2 accumulated, EFS contractions decreased with time, and EJPs disappeared. We conclude that in canine bronchi PGE2 predominantly inhibits ACh release and endogenous PGE2 acts similarly, whereas TxA2 excites, probably at postjunctional sites.
ISSN:0002-9513
DOI:10.1152/ajplung.1995.268.1.l47