Journal of Applied Physiology, Vol 63, Issue 6 2309-2314, Copyright © 1987 by American Physiological Society
Cyclic nucleotide function in trachealis muscle of dogs with and without airway hyperresponsiveness
D. R. Austin, S. C. Chan, J. M. Hanifin, H. Downes, C. Parks and C. A. Hirshman
Department of Anesthesiology, Oregon Health Sciences University, Portland 97201.
We examined basal adenosine 3',5'-cyclic monophosphate (cAMP) levels,
isoproterenol (ISO)-stimulated cAMP responses, basal cAMP, and guanosine
3',5'-cyclic monophosphate (cGMP) phosphodiesterase (PDE) activities and
protein-kinase (PK) activities in trachealis muscle from five
Basenji-greyhound (BG) and four greyhound dogs to determine whether the
inverse relationship between in vivo and in vitro airway responsiveness
could be due to altered cyclic nucleotide metabolism. Basal cAMP levels
were not significantly different (PNS) in muscle from BG (11.6 +/- 0.53
pmol/mg protein) and greyhound dogs (10.30 +/- 1.60 pmol/mg protein). The
cAMP responses to stimulation with ISO were enhanced in BG compared with
greyhound dogs. The low Michaelis constant (1) for Km-cAMP PDE activity (Km
= 0.63 microM) was significantly less (P less than 0.005) in BG dogs (1.54
+/- 0.28 pmol.min-1.mg protein-1) than greyhounds (11.76 +/- 2.48).
Endogenously active PK activity was significantly greater (P less than
0.005) in BG (54.74 +/- 5.39 pmol.min-1.mg protein-1) than in greyhound
dogs (15.50 +/0 2.20). Increases in PK activity with 5 microM cAMP added
were not significantly different between BG (14.79 +/- 6.00) and greyhound
dogs (7.04 +/- 2.14). Approximately 90% of both endogenous PK activity and
cAMP-activated PK activity in BG and greyhound dogs was inhibited by a
cAMP-dependent PK inhibitor (PKI'). These data suggest that decreased
cyclic nucleotide degradation due to decreased cyclic nucleotide PDE
activity with increased PK could account for the in vitro
hyporesponsiveness of airway smooth muscle in BG dogs as a protective
adaptive mechanism.
