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Pharmacological Features of Vascular Responses of Isolated Dog and Monkey Lingual Arteries to Vasoactive Substances
[摘要] References(27)Cited-By(14)Using a perfusion technique of isolated vessels, vasoconstrictor responses to alpha adrenoceptor agonists (norepinephrine [NE], phenylephrine [PE], clonidine, xylazine and tyramine) and KCl were investigated in isolated, perfused dog and monkey lingual arteries. A stainless steel cannula was inserted into the lingual artery segment and perfused with Krebs-Henseleit solution at a constant flow rate. In dog lingual avteries, the agonists induced vasoconstrictions with the following order of potency: NE > PE > tyramine >> clonidine > xylazine > KCl. In monkey preparations, the order was NE > PE >> clonidine ≥ tyramine > xylazine > KCl. In both preparations, NE- and PE-induced constrictions were blocked by bunazosin (an alpha-1 adrenoceptor antagonist), but not influenced by midaglizole (a potent alpha-2 antagonist). Diltiazem (a Ca entry blocker) significantly attenuated NE-induced vasoconstrictions in dog lingual arteries, but did not significantly influence these in monkey preparations. These results suggest that: [1] these arteries contain mostly alpha-1 but scarcely any alpha-2 adrenoceptors; [2] in dog preparations, tyramine induced a marked vasoconstriction which may contribute to investigation on the mechanisms of catecholamine releases from sympathetic nerve terminals; and [3] different blocking effects of diltiazem may indicate that extracellular Ca++ influx may have varying degrees of importance in alpha-1 adrenoreceptor-mediated constrictions in different species, although participation of an intracellular mechanism might not be ruled out.
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[效力级别]  [学科分类] 药理学
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