A study comparing biopharmaceutic characteristics of four once daily controlled release diltiazem preparations

Summary— In the present study we have compared the steady state biopharmaceutic characteristics of four diltiazem once daily controlled release capsules: Mono‐Tildiem LP 300® (300 mg), Adizem® XL (300 mg)1, Cardizem® (300 mg) and Dilacor® (240 mg). Sixteen healthy male volunteers (aged 22.9 ± 3.3 ye...

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Published in:Fundamental & clinical pharmacology 1998-01, Vol.12 (5), p.559-565
Main Authors: Hendriks, MGC, Dogterom, P, Ebels, JT, Oosterhuis, B, Geertsema, LR, Hulot, T, Bianchetti, G, Jonkman, JHG
Format: Article
Language:English
Subjects:
Adult
Antianginal agents. Coronary vasodilator agents
Area Under Curve
Biological and medical sciences
biopharmaceutics
Calcium Channel Blockers - blood
Calcium Channel Blockers - pharmacokinetics
Cardiovascular system
controlled release
Cross-Over Studies
Delayed-Action Preparations
diltiazem
Diltiazem - blood
Diltiazem - pharmacokinetics
Humans
Male
Medical sciences
Pharmacology. Drug treatments
plasma profiles
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cited_by cdi_FETCH-LOGICAL-c4366-a73a1f86dd88cd3566a06c5666ea3a3e8bd60750773999d5d56081694eb136f83
cites cdi_FETCH-LOGICAL-c4366-a73a1f86dd88cd3566a06c5666ea3a3e8bd60750773999d5d56081694eb136f83
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container_issue 5
container_start_page 559
container_title Fundamental & clinical pharmacology
container_volume 12
creator Hendriks, MGC
Dogterom, P
Ebels, JT
Oosterhuis, B
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Bianchetti, G
Jonkman, JHG
description Summary— In the present study we have compared the steady state biopharmaceutic characteristics of four diltiazem once daily controlled release capsules: Mono‐Tildiem LP 300® (300 mg), Adizem® XL (300 mg)1, Cardizem® (300 mg) and Dilacor® (240 mg). Sixteen healthy male volunteers (aged 22.9 ± 3.3 years, range 19–31 years) completed an open label, multiple oral dose, randomized, four‐period crossover study without a washout period in between. The volunteers received each diltiazem formulation once daily for four days. Trough diltiazem and metabolites plasma concentrations were determined on days 3 and 4. The 24‐h plasma concentration‐time profiles were assessed after the dose on day 4 of each period. The following steady state pharmacokinetic parameters for diltiazem were calculated: the minimum plasma concentration (cmin), the maximum plasma concentration (cmax), the time to reach that concentration (tmax), the time interval during which the plasma concentration exceeds 50% of cmax (t50), the area under the plasma concentration‐time curve (AUC72–96) and the peak‐to‐trough fluctuation (PTF). For the metabolites of diltiazem, N‐mono‐desmethyl‐diltiazem (NDM) and desacetyldiltiazem (DAD), AUC72–96 (AUCNDM and AUCDAD) and the ratio metabolite/parent compound were calculated. Steady state was achieved on day 3. Except one, all controlled release formulations have satisfactory controlled release properties allowing once daily administration. However, significant (P < 0.05) differences were found between the pharmacokinetic characteristics which do not allow exchange of the various formulations. Concentrations well below 50 ng·mL‐1 in the morning hours were observed for Dilacor® (240 mg) and Adizem® XL (300 mg), which could be a disadvantage of these formulations as it is well‐known that ischaemic events occur at a higher rate during that part of the day. The plasma concentration profiles of NDM and DAD, the major circulating metabolites, parallel the plasma concentration profiles for the parent compound. From a clinical point of view, all treatments were well tolerated.
doi_str_mv 10.1111/j.1472-8206.1998.tb00986.x
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Sixteen healthy male volunteers (aged 22.9 ± 3.3 years, range 19–31 years) completed an open label, multiple oral dose, randomized, four‐period crossover study without a washout period in between. The volunteers received each diltiazem formulation once daily for four days. Trough diltiazem and metabolites plasma concentrations were determined on days 3 and 4. The 24‐h plasma concentration‐time profiles were assessed after the dose on day 4 of each period. The following steady state pharmacokinetic parameters for diltiazem were calculated: the minimum plasma concentration (cmin), the maximum plasma concentration (cmax), the time to reach that concentration (tmax), the time interval during which the plasma concentration exceeds 50% of cmax (t50), the area under the plasma concentration‐time curve (AUC72–96) and the peak‐to‐trough fluctuation (PTF). For the metabolites of diltiazem, N‐mono‐desmethyl‐diltiazem (NDM) and desacetyldiltiazem (DAD), AUC72–96 (AUCNDM and AUCDAD) and the ratio metabolite/parent compound were calculated. Steady state was achieved on day 3. Except one, all controlled release formulations have satisfactory controlled release properties allowing once daily administration. However, significant (P &lt; 0.05) differences were found between the pharmacokinetic characteristics which do not allow exchange of the various formulations. Concentrations well below 50 ng·mL‐1 in the morning hours were observed for Dilacor® (240 mg) and Adizem® XL (300 mg), which could be a disadvantage of these formulations as it is well‐known that ischaemic events occur at a higher rate during that part of the day. The plasma concentration profiles of NDM and DAD, the major circulating metabolites, parallel the plasma concentration profiles for the parent compound. 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Sixteen healthy male volunteers (aged 22.9 ± 3.3 years, range 19–31 years) completed an open label, multiple oral dose, randomized, four‐period crossover study without a washout period in between. The volunteers received each diltiazem formulation once daily for four days. Trough diltiazem and metabolites plasma concentrations were determined on days 3 and 4. The 24‐h plasma concentration‐time profiles were assessed after the dose on day 4 of each period. The following steady state pharmacokinetic parameters for diltiazem were calculated: the minimum plasma concentration (cmin), the maximum plasma concentration (cmax), the time to reach that concentration (tmax), the time interval during which the plasma concentration exceeds 50% of cmax (t50), the area under the plasma concentration‐time curve (AUC72–96) and the peak‐to‐trough fluctuation (PTF). For the metabolites of diltiazem, N‐mono‐desmethyl‐diltiazem (NDM) and desacetyldiltiazem (DAD), AUC72–96 (AUCNDM and AUCDAD) and the ratio metabolite/parent compound were calculated. Steady state was achieved on day 3. Except one, all controlled release formulations have satisfactory controlled release properties allowing once daily administration. However, significant (P &lt; 0.05) differences were found between the pharmacokinetic characteristics which do not allow exchange of the various formulations. Concentrations well below 50 ng·mL‐1 in the morning hours were observed for Dilacor® (240 mg) and Adizem® XL (300 mg), which could be a disadvantage of these formulations as it is well‐known that ischaemic events occur at a higher rate during that part of the day. The plasma concentration profiles of NDM and DAD, the major circulating metabolites, parallel the plasma concentration profiles for the parent compound. 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Sixteen healthy male volunteers (aged 22.9 ± 3.3 years, range 19–31 years) completed an open label, multiple oral dose, randomized, four‐period crossover study without a washout period in between. The volunteers received each diltiazem formulation once daily for four days. Trough diltiazem and metabolites plasma concentrations were determined on days 3 and 4. The 24‐h plasma concentration‐time profiles were assessed after the dose on day 4 of each period. The following steady state pharmacokinetic parameters for diltiazem were calculated: the minimum plasma concentration (cmin), the maximum plasma concentration (cmax), the time to reach that concentration (tmax), the time interval during which the plasma concentration exceeds 50% of cmax (t50), the area under the plasma concentration‐time curve (AUC72–96) and the peak‐to‐trough fluctuation (PTF). For the metabolites of diltiazem, N‐mono‐desmethyl‐diltiazem (NDM) and desacetyldiltiazem (DAD), AUC72–96 (AUCNDM and AUCDAD) and the ratio metabolite/parent compound were calculated. Steady state was achieved on day 3. Except one, all controlled release formulations have satisfactory controlled release properties allowing once daily administration. However, significant (P &lt; 0.05) differences were found between the pharmacokinetic characteristics which do not allow exchange of the various formulations. Concentrations well below 50 ng·mL‐1 in the morning hours were observed for Dilacor® (240 mg) and Adizem® XL (300 mg), which could be a disadvantage of these formulations as it is well‐known that ischaemic events occur at a higher rate during that part of the day. The plasma concentration profiles of NDM and DAD, the major circulating metabolites, parallel the plasma concentration profiles for the parent compound. 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source Wiley-Blackwell Read & Publish Collection
subjects Adult
Antianginal agents. Coronary vasodilator agents
Area Under Curve
Biological and medical sciences
biopharmaceutics
Calcium Channel Blockers - blood
Calcium Channel Blockers - pharmacokinetics
Cardiovascular system
controlled release
Cross-Over Studies
Delayed-Action Preparations
diltiazem
Diltiazem - blood
Diltiazem - pharmacokinetics
Humans
Male
Medical sciences
Pharmacology. Drug treatments
plasma profiles
title A study comparing biopharmaceutic characteristics of four once daily controlled release diltiazem preparations
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