Clinical pharmacology of doxazosin in patients with essential hypertension

Luigi X. Cubeddu; Nery Fuenmayor; Nancy Caplan; Donald Ferry

doi:10.1038/clpt.1987.54

Clinical pharmacology of doxazosin in patients with essential hypertension

Luigi X. Cubeddu
, Nery Fuenmayor
, Nancy Caplan
, Donald Ferry

Research output: Contribution to journal › Article › peer-review

51 Scopus citations

Abstract

Doxazosin is a new quinazoline derivative that, like prazosin, has selectivity forα1-receptors. A three-way crossover, randomized, open study in 18 patients with essential hypertension was conducted to investigate the clinical pharmacokinetics of 2, 4, and 8 mg doxazosin at steady state. The pharmacokinetics of the initial 2 mg dose was also studied. Doxazosin showed linear pharmacokinetics. Increases in doses from 2 to 8 mg (steady state) produced proportional increases in doxazosin serum levels (maximum plasma drug concentration [Cmax] minimum plasma drug concentration [Cmin], and O-24-hour area under the curve [AUC(p-24)], whereas half-life (t 1 2) (19.4, 18.7, and 19.7 hours, respectively), volume of distribution (3.4, 3.4, and 3.6 L/kg, respectively), clearance from serum (2.2, 2.2, and 2.1 ml/min/kg, respectively), and degree of protein binding (1.2%, 1.0%, and 1.0% unbound, respectively) were dose independent. Similar t 1 2) and time to reach peak concentration (tmax) were obtained with 2 mg initial dose and 2 mg steady state. α1-Acid glycoprotein levels were unchanged during doxazosin treatment. Doxazosin lowered supine and standing systolic and diastolic blood pressure. The blood pressure reduction was associated with an increase in heart rate. Peak hypotensive and tachycardic effects occurred 5.7 ± 0.1 hours after administration, whereas Cmax was achieved at 2.4 ± 0.7 hours (tmax). Greater decreases in systolic blood pressure and increases in heart rate were seen in standing than in supine position. The reduction in standing systolic and diastolic blood pressure with 8 mg was greater than with 2 mg (P < 0.05); however, the increases in heart rate were not different. Dizziness, headaches, and dry mouth were the most frequent side effects. This study indicates that doxazosin shows linear pharmacokinetics between 2 and 8 mg and that because of its long t 1 2), once-a-day administration should be adequate for the treatment of hypertension.

Original language	English
Pages (from-to)	439-449
Number of pages	11
Journal	Clinical Pharmacology and Therapeutics
Volume	41
Issue number	4
DOIs	https://doi.org/10.1038/clpt.1987.54
State	Published - Apr 1987
Externally published	Yes

ASJC Scopus Subject Areas

Pharmacology
Pharmacology (medical)

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10.1038/clpt.1987.54

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title = "Clinical pharmacology of doxazosin in patients with essential hypertension",

abstract = "Doxazosin is a new quinazoline derivative that, like prazosin, has selectivity forα1-receptors. A three-way crossover, randomized, open study in 18 patients with essential hypertension was conducted to investigate the clinical pharmacokinetics of 2, 4, and 8 mg doxazosin at steady state. The pharmacokinetics of the initial 2 mg dose was also studied. Doxazosin showed linear pharmacokinetics. Increases in doses from 2 to 8 mg (steady state) produced proportional increases in doxazosin serum levels (maximum plasma drug concentration [Cmax] minimum plasma drug concentration [Cmin], and O-24-hour area under the curve [AUC(p-24)], whereas half-life (t 1 2) (19.4, 18.7, and 19.7 hours, respectively), volume of distribution (3.4, 3.4, and 3.6 L/kg, respectively), clearance from serum (2.2, 2.2, and 2.1 ml/min/kg, respectively), and degree of protein binding (1.2\%, 1.0\%, and 1.0\% unbound, respectively) were dose independent. Similar t 1 2) and time to reach peak concentration (tmax) were obtained with 2 mg initial dose and 2 mg steady state. α1-Acid glycoprotein levels were unchanged during doxazosin treatment. Doxazosin lowered supine and standing systolic and diastolic blood pressure. The blood pressure reduction was associated with an increase in heart rate. Peak hypotensive and tachycardic effects occurred 5.7 ± 0.1 hours after administration, whereas Cmax was achieved at 2.4 ± 0.7 hours (tmax). Greater decreases in systolic blood pressure and increases in heart rate were seen in standing than in supine position. The reduction in standing systolic and diastolic blood pressure with 8 mg was greater than with 2 mg (P < 0.05); however, the increases in heart rate were not different. Dizziness, headaches, and dry mouth were the most frequent side effects. This study indicates that doxazosin shows linear pharmacokinetics between 2 and 8 mg and that because of its long t 1 2), once-a-day administration should be adequate for the treatment of hypertension.",

author = "Cubeddu, \{Luigi X.\} and Nery Fuenmayor and Nancy Caplan and Donald Ferry",

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AU - Cubeddu, Luigi X.

AU - Fuenmayor, Nery

AU - Caplan, Nancy

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N2 - Doxazosin is a new quinazoline derivative that, like prazosin, has selectivity forα1-receptors. A three-way crossover, randomized, open study in 18 patients with essential hypertension was conducted to investigate the clinical pharmacokinetics of 2, 4, and 8 mg doxazosin at steady state. The pharmacokinetics of the initial 2 mg dose was also studied. Doxazosin showed linear pharmacokinetics. Increases in doses from 2 to 8 mg (steady state) produced proportional increases in doxazosin serum levels (maximum plasma drug concentration [Cmax] minimum plasma drug concentration [Cmin], and O-24-hour area under the curve [AUC(p-24)], whereas half-life (t 1 2) (19.4, 18.7, and 19.7 hours, respectively), volume of distribution (3.4, 3.4, and 3.6 L/kg, respectively), clearance from serum (2.2, 2.2, and 2.1 ml/min/kg, respectively), and degree of protein binding (1.2%, 1.0%, and 1.0% unbound, respectively) were dose independent. Similar t 1 2) and time to reach peak concentration (tmax) were obtained with 2 mg initial dose and 2 mg steady state. α1-Acid glycoprotein levels were unchanged during doxazosin treatment. Doxazosin lowered supine and standing systolic and diastolic blood pressure. The blood pressure reduction was associated with an increase in heart rate. Peak hypotensive and tachycardic effects occurred 5.7 ± 0.1 hours after administration, whereas Cmax was achieved at 2.4 ± 0.7 hours (tmax). Greater decreases in systolic blood pressure and increases in heart rate were seen in standing than in supine position. The reduction in standing systolic and diastolic blood pressure with 8 mg was greater than with 2 mg (P < 0.05); however, the increases in heart rate were not different. Dizziness, headaches, and dry mouth were the most frequent side effects. This study indicates that doxazosin shows linear pharmacokinetics between 2 and 8 mg and that because of its long t 1 2), once-a-day administration should be adequate for the treatment of hypertension.

AB - Doxazosin is a new quinazoline derivative that, like prazosin, has selectivity forα1-receptors. A three-way crossover, randomized, open study in 18 patients with essential hypertension was conducted to investigate the clinical pharmacokinetics of 2, 4, and 8 mg doxazosin at steady state. The pharmacokinetics of the initial 2 mg dose was also studied. Doxazosin showed linear pharmacokinetics. Increases in doses from 2 to 8 mg (steady state) produced proportional increases in doxazosin serum levels (maximum plasma drug concentration [Cmax] minimum plasma drug concentration [Cmin], and O-24-hour area under the curve [AUC(p-24)], whereas half-life (t 1 2) (19.4, 18.7, and 19.7 hours, respectively), volume of distribution (3.4, 3.4, and 3.6 L/kg, respectively), clearance from serum (2.2, 2.2, and 2.1 ml/min/kg, respectively), and degree of protein binding (1.2%, 1.0%, and 1.0% unbound, respectively) were dose independent. Similar t 1 2) and time to reach peak concentration (tmax) were obtained with 2 mg initial dose and 2 mg steady state. α1-Acid glycoprotein levels were unchanged during doxazosin treatment. Doxazosin lowered supine and standing systolic and diastolic blood pressure. The blood pressure reduction was associated with an increase in heart rate. Peak hypotensive and tachycardic effects occurred 5.7 ± 0.1 hours after administration, whereas Cmax was achieved at 2.4 ± 0.7 hours (tmax). Greater decreases in systolic blood pressure and increases in heart rate were seen in standing than in supine position. The reduction in standing systolic and diastolic blood pressure with 8 mg was greater than with 2 mg (P < 0.05); however, the increases in heart rate were not different. Dizziness, headaches, and dry mouth were the most frequent side effects. This study indicates that doxazosin shows linear pharmacokinetics between 2 and 8 mg and that because of its long t 1 2), once-a-day administration should be adequate for the treatment of hypertension.

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Clinical pharmacology of doxazosin in patients with essential hypertension

Abstract

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