Studies on the Cardiovascular Effects of Pindolol in Doca/Saline Hypertensive Rats

Abstract: 1 A hypotensive response to orally administered pindolol in conscious normotensive and deoxycorticosterone acetate (DOCA)/saline hypertensive rats (DS‐rats) is described. In DS‐rats, pindolol (10‐50 μg/kg) produced a dose‐dependent fall in blood pressure and elevation of resting heart rate. 2 The hypotensive response and tachycardia produced by oral pindolol (50 μg/kg) in DS‐rats were prevented by propranolol (5 mg/kg), suggesting that pindolol's effects are mediated by β‐adrenoceptor stimulation. 3 After meca… Show more

“…Introduction The non-selective fl-adrenoceptor blocking drug, pindolol, has been shown to lower the blood pressure of deoxycorticosterone acetate (DOCA)-saline hypertensive (DS) rats after oral administration of small doses (Buckingham, Hamilton & Robson, 1977). The effect was dose-related and appeared to be mediated by a metabolite(s) acting by stimulation of vascular fi2-adrenoceptors.…”

“…Pindolol is extensively metabolized in rats (Kiechel, Niklaus, Schreier & Wagner, 1975) and has a short plasma half life after oral administration (Pacha, 1969). Our earlier studies (Buckingham et al, 1977) suggested that the hypotensive response to pindolol in the DS-rat is mediated through a metabolite(s) formed predominantly in the liver. Over-loading of the hepatic extraction process, by administration of a sufficiently large oral dose, would reduce the fraction of drug removed on its first passage through the liver, as occurs with propranolol in the rat (Shand, Rangno, & Evans, 1972).…”

“…Over-loading of the hepatic extraction process, by administration of a sufficiently large oral dose, would reduce the fraction of drug removed on its first passage through the liver, as occurs with propranolol in the rat (Shand, Rangno, & Evans, 1972). Since the hypotensive effect in the DS-rat is apparently due to stimulation of vascular /2-receptors (Buckingham et al, 1977) an increase in the fraction of circulating parent drug, with its inherent f3-adrenoceptor blocking properties, might be expected to attenuate the response. Subsequent metabolism of the parent drug would account for the diminution of differences in effect of the three pindolol doses at 3 and 4 hours.…”

“…Methods DS-rats were prepared by the method previously described (Buckingham et al, 1977). In some rats unilateral adrenalectomy and contralateral adrenal demedullation were performed at this operation (adrenal demedullated DS-rats).…”

Diminishing Hypotensive Effect of Increasing Doses of Pindolol in Doca/Saline Hypertensive Rats

“…Introduction The non-selective fl-adrenoceptor blocking drug, pindolol, has been shown to lower the blood pressure of deoxycorticosterone acetate (DOCA)-saline hypertensive (DS) rats after oral administration of small doses (Buckingham, Hamilton & Robson, 1977). The effect was dose-related and appeared to be mediated by a metabolite(s) acting by stimulation of vascular fi2-adrenoceptors.…”

“…Pindolol is extensively metabolized in rats (Kiechel, Niklaus, Schreier & Wagner, 1975) and has a short plasma half life after oral administration (Pacha, 1969). Our earlier studies (Buckingham et al, 1977) suggested that the hypotensive response to pindolol in the DS-rat is mediated through a metabolite(s) formed predominantly in the liver. Over-loading of the hepatic extraction process, by administration of a sufficiently large oral dose, would reduce the fraction of drug removed on its first passage through the liver, as occurs with propranolol in the rat (Shand, Rangno, & Evans, 1972).…”

“…Over-loading of the hepatic extraction process, by administration of a sufficiently large oral dose, would reduce the fraction of drug removed on its first passage through the liver, as occurs with propranolol in the rat (Shand, Rangno, & Evans, 1972). Since the hypotensive effect in the DS-rat is apparently due to stimulation of vascular /2-receptors (Buckingham et al, 1977) an increase in the fraction of circulating parent drug, with its inherent f3-adrenoceptor blocking properties, might be expected to attenuate the response. Subsequent metabolism of the parent drug would account for the diminution of differences in effect of the three pindolol doses at 3 and 4 hours.…”

“…Methods DS-rats were prepared by the method previously described (Buckingham et al, 1977). In some rats unilateral adrenalectomy and contralateral adrenal demedullation were performed at this operation (adrenal demedullated DS-rats).…”

Diminishing Hypotensive Effect of Increasing Doses of Pindolol in Doca/Saline Hypertensive Rats

“…Although metabolites of pindolol have been found to be pharmacologically active in the rat (Buckingham et al, 1977), no evidence of active metabolites of pindolol in man has been forthcoming (Aellig, 1976b). Although similar oral and intravenous doses produce the same 0-adrenoceptor blockade (Carruthers, 1982), there has never been any comparison of the plasma concentration-response relationships of pindolol after oral and intravenous administration in the manner described for oral and intravenous propranolol by Cleaveland & Shand (1972).…”

Contrasts between pindolol and propranolol concentration‐response relationships.

Effects on the General Hemodynamics and Peripheral Circulation