TY - JOUR
T1 - Effects of CRL 41034 on the adrenergic neuroeffector interaction in the canine saphenous vein
AU - Boulanger, C.
AU - Flavahan, NA
AU - Katusic, ZS
AU - Komori, K.
AU - Vos, AA
AU - Vanhoutte, PM
PY - 1990
Y1 - 1990
N2 - Summary— Experiments were designed to determine the effect of CRL 41034, a buflomedil analogue, on the adrenergic responsiveness of canine veins. Rings of saphenous vein (without endothelium) were suspended for isometric tension recording in modified Krebs‐Ringer bicarbonate solution at 37°C. CRL 41034 produced a concentration‐dependent inhibition of the contractions evoked by the alpha adrenergic agonists norepinephrine, phenylephrine and UK 14304 which was insensitive to the blockade of neuronal uptake by cocaine. CRL 41034 was more potent in inhibiting the concentration‐dependent contractions evoked by UK 14304 than those by phenylephrine and the antagonism it caused against the response to UK 14304 fulfilled the criteria for competitivity. CRL 41034, at 10−5 M significantly depressed, and at 10−4 M abolished the contractions induced by electrical stimulation of the adrenergic nerves and those evoked by the indirect sympathomimetic amine tyramine. Strips of canine saphenous vein were superfused after incubation with [3H] norepinephrine. During sympathetic nerve activation, CRL 41304 increased the stimulation‐evoked overflow of [3H] norepinephrine and 3‐methoxy‐4‐dihydroxyphenylglycol; in the presence of rauwolscine the compound only increased the stimulation‐evoked overflow of 3,4‐dihydroxyphenylglycol. These experiments suggest that the major vascular effects of CRL 41034 in canine veins are blockade of alpha2‐adrenoceptors on vascular smooth muscle, and inhibition of prejunctional alpha2‐adrenoceptors on adrenergic nerve endings. 1990 Société Française de Pharmacologie et de Thérapeutique
AB - Summary— Experiments were designed to determine the effect of CRL 41034, a buflomedil analogue, on the adrenergic responsiveness of canine veins. Rings of saphenous vein (without endothelium) were suspended for isometric tension recording in modified Krebs‐Ringer bicarbonate solution at 37°C. CRL 41034 produced a concentration‐dependent inhibition of the contractions evoked by the alpha adrenergic agonists norepinephrine, phenylephrine and UK 14304 which was insensitive to the blockade of neuronal uptake by cocaine. CRL 41034 was more potent in inhibiting the concentration‐dependent contractions evoked by UK 14304 than those by phenylephrine and the antagonism it caused against the response to UK 14304 fulfilled the criteria for competitivity. CRL 41034, at 10−5 M significantly depressed, and at 10−4 M abolished the contractions induced by electrical stimulation of the adrenergic nerves and those evoked by the indirect sympathomimetic amine tyramine. Strips of canine saphenous vein were superfused after incubation with [3H] norepinephrine. During sympathetic nerve activation, CRL 41304 increased the stimulation‐evoked overflow of [3H] norepinephrine and 3‐methoxy‐4‐dihydroxyphenylglycol; in the presence of rauwolscine the compound only increased the stimulation‐evoked overflow of 3,4‐dihydroxyphenylglycol. These experiments suggest that the major vascular effects of CRL 41034 in canine veins are blockade of alpha2‐adrenoceptors on vascular smooth muscle, and inhibition of prejunctional alpha2‐adrenoceptors on adrenergic nerve endings. 1990 Société Française de Pharmacologie et de Thérapeutique
KW - adrenergic neurotransmission
KW - buflomedil
KW - release of norepinephrine
KW - subtypes of alpha adrenergic receptors
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U2 - 10.1111/j.1472-8206.1990.tb00037.x
DO - 10.1111/j.1472-8206.1990.tb00037.x
M3 - Article
C2 - 1981202
AN - SCOPUS:0025197391
SN - 0767-3981
VL - 4
SP - 525
EP - 538
JO - Fundamental and Clinical Pharmacology
JF - Fundamental and Clinical Pharmacology
IS - 5
ER -