Nonlinear kinetics and pharmacologic response to mibefradil
Background Increasing oral doses of mibefradil (10 to 320 mg) decrease its apparent oral clearance; however, intravenous doses up to 80 mg do not reduce its systemic clearance. This study aimed to understand the mechanisms underlying the zero‐order kinetics of mibefradil. Methods A group of 10 normo...
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| creator | Souich, Patrick Besner, Jean‐Guy Clozel, Jean‐Paul Welker, Horst A. Lefebvre, Marc Caillé, Gilles |
| description | Background
Increasing oral doses of mibefradil (10 to 320 mg) decrease its apparent oral clearance; however, intravenous doses up to 80 mg do not reduce its systemic clearance. This study aimed to understand the mechanisms underlying the zero‐order kinetics of mibefradil.
Methods
A group of 10 normotensive volunteers received 50 mg/day oral mibefradil for 8 days and, on days 1 and 8, 5 mg deuterated mibefradil by infusion. Ten additional volunteers observed the same protocol with a daily oral dose of 100 mg mibefradil. Serial blood samples were withdrawn, and mibefradil plasma concentrations were assayed by liquid chromatography–mass spectrometry. Blood pressure and heart rate were measured for 4 hours, and an ECG was performed 2 hours after drug administration.
Results
Repeated oral administration of 50 mg mibefradil generated zero‐order kinetics secondary to a decrease in mibefradil systemic clearance. Compared with the 50‐mg dose, single and repeated oral doses of 100 mg further decreased mibefradil clearance. Mibefradil bioavailability was not affected by increasing mibefradil doses. Mean diastolic blood pressure was decreased by single and repeated doses of 100 mg to the same extent. Repeated doses of 100 mg reduced heart rate and prolonged the PR and QTc, changes that were associated with mibefradil plasma concentrations.
Conclusions
Repeated doses of 50 mg or doses of 100 mg mibefradil generated zero‐order kinetics secondary to a decrease in hepatic extraction of the drug. Zero‐order kinetics did not affect the response‐concentration relationship of mibefradil. (Clin Pharmacol Ther 2000;67:249–57.)
Clinical Pharmacology & Therapeutics (2000) 67, 249–257; doi: 10.1067/mcp.2000.104616 |
| doi_str_mv | 10.1067/mcp.2000.104616 |
| format | Article |
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Increasing oral doses of mibefradil (10 to 320 mg) decrease its apparent oral clearance; however, intravenous doses up to 80 mg do not reduce its systemic clearance. This study aimed to understand the mechanisms underlying the zero‐order kinetics of mibefradil.
Methods
A group of 10 normotensive volunteers received 50 mg/day oral mibefradil for 8 days and, on days 1 and 8, 5 mg deuterated mibefradil by infusion. Ten additional volunteers observed the same protocol with a daily oral dose of 100 mg mibefradil. Serial blood samples were withdrawn, and mibefradil plasma concentrations were assayed by liquid chromatography–mass spectrometry. Blood pressure and heart rate were measured for 4 hours, and an ECG was performed 2 hours after drug administration.
Results
Repeated oral administration of 50 mg mibefradil generated zero‐order kinetics secondary to a decrease in mibefradil systemic clearance. Compared with the 50‐mg dose, single and repeated oral doses of 100 mg further decreased mibefradil clearance. Mibefradil bioavailability was not affected by increasing mibefradil doses. Mean diastolic blood pressure was decreased by single and repeated doses of 100 mg to the same extent. Repeated doses of 100 mg reduced heart rate and prolonged the PR and QTc, changes that were associated with mibefradil plasma concentrations.
Conclusions
Repeated doses of 50 mg or doses of 100 mg mibefradil generated zero‐order kinetics secondary to a decrease in hepatic extraction of the drug. Zero‐order kinetics did not affect the response‐concentration relationship of mibefradil. (Clin Pharmacol Ther 2000;67:249–57.)
Clinical Pharmacology & Therapeutics (2000) 67, 249–257; doi: 10.1067/mcp.2000.104616</description><identifier>ISSN: 0009-9236</identifier><identifier>EISSN: 1532-6535</identifier><identifier>DOI: 10.1067/mcp.2000.104616</identifier><identifier>PMID: 10741628</identifier><identifier>CODEN: CLPTAT</identifier><language>eng</language><publisher>New York, NY: Nature Publishing</publisher><subject>Administration, Oral ; Adult ; Antihypertensive agents ; Antihypertensive Agents - administration & dosage ; Antihypertensive Agents - blood ; Antihypertensive Agents - pharmacokinetics ; Antihypertensive Agents - pharmacology ; Biological and medical sciences ; Biological Availability ; Cardiovascular system ; Drug Administration Schedule ; Gas Chromatography-Mass Spectrometry ; Heart Conduction System - drug effects ; Heart Rate - drug effects ; Humans ; Infusions, Intravenous ; Male ; Medical sciences ; Mibefradil - administration & dosage ; Mibefradil - blood ; Mibefradil - pharmacokinetics ; Mibefradil - pharmacology ; Pharmacology. Drug treatments ; Reference Values</subject><ispartof>Clinical pharmacology and therapeutics, 2000-03, Vol.67 (3), p.249-257</ispartof><rights>2000 American Society for Clinical Pharmacology and Therapeutics</rights><rights>2000 INIST-CNRS</rights><lds50>peer_reviewed</lds50><woscitedreferencessubscribed>false</woscitedreferencessubscribed><citedby>FETCH-LOGICAL-c3989-1fbc67f891187e8ecf031d73506897101c3138ce2c1c9b1ea9093f3b81506fcb3</citedby></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><linktopdf>$$Uhttps://onlinelibrary.wiley.com/doi/pdf/10.1067%2Fmcp.2000.104616$$EPDF$$P50$$Gwiley$$H</linktopdf><linktohtml>$$Uhttps://onlinelibrary.wiley.com/doi/full/10.1067%2Fmcp.2000.104616$$EHTML$$P50$$Gwiley$$H</linktohtml><link.rule.ids>314,780,784,1417,27924,27925,45574,45575</link.rule.ids><backlink>$$Uhttp://pascal-francis.inist.fr/vibad/index.php?action=getRecordDetail&idt=1331982$$DView record in Pascal Francis$$Hfree_for_read</backlink><backlink>$$Uhttps://www.ncbi.nlm.nih.gov/pubmed/10741628$$D View this record in MEDLINE/PubMed$$Hfree_for_read</backlink></links><search><creatorcontrib>Souich, Patrick</creatorcontrib><creatorcontrib>Besner, Jean‐Guy</creatorcontrib><creatorcontrib>Clozel, Jean‐Paul</creatorcontrib><creatorcontrib>Welker, Horst A.</creatorcontrib><creatorcontrib>Lefebvre, Marc</creatorcontrib><creatorcontrib>Caillé, Gilles</creatorcontrib><title>Nonlinear kinetics and pharmacologic response to mibefradil</title><title>Clinical pharmacology and therapeutics</title><addtitle>Clin Pharmacol Ther</addtitle><description>Background
Increasing oral doses of mibefradil (10 to 320 mg) decrease its apparent oral clearance; however, intravenous doses up to 80 mg do not reduce its systemic clearance. This study aimed to understand the mechanisms underlying the zero‐order kinetics of mibefradil.
Methods
A group of 10 normotensive volunteers received 50 mg/day oral mibefradil for 8 days and, on days 1 and 8, 5 mg deuterated mibefradil by infusion. Ten additional volunteers observed the same protocol with a daily oral dose of 100 mg mibefradil. Serial blood samples were withdrawn, and mibefradil plasma concentrations were assayed by liquid chromatography–mass spectrometry. Blood pressure and heart rate were measured for 4 hours, and an ECG was performed 2 hours after drug administration.
Results
Repeated oral administration of 50 mg mibefradil generated zero‐order kinetics secondary to a decrease in mibefradil systemic clearance. Compared with the 50‐mg dose, single and repeated oral doses of 100 mg further decreased mibefradil clearance. Mibefradil bioavailability was not affected by increasing mibefradil doses. Mean diastolic blood pressure was decreased by single and repeated doses of 100 mg to the same extent. Repeated doses of 100 mg reduced heart rate and prolonged the PR and QTc, changes that were associated with mibefradil plasma concentrations.
Conclusions
Repeated doses of 50 mg or doses of 100 mg mibefradil generated zero‐order kinetics secondary to a decrease in hepatic extraction of the drug. Zero‐order kinetics did not affect the response‐concentration relationship of mibefradil. (Clin Pharmacol Ther 2000;67:249–57.)
Clinical Pharmacology & Therapeutics (2000) 67, 249–257; doi: 10.1067/mcp.2000.104616</description><subject>Administration, Oral</subject><subject>Adult</subject><subject>Antihypertensive agents</subject><subject>Antihypertensive Agents - administration & dosage</subject><subject>Antihypertensive Agents - blood</subject><subject>Antihypertensive Agents - pharmacokinetics</subject><subject>Antihypertensive Agents - pharmacology</subject><subject>Biological and medical sciences</subject><subject>Biological Availability</subject><subject>Cardiovascular system</subject><subject>Drug Administration Schedule</subject><subject>Gas Chromatography-Mass Spectrometry</subject><subject>Heart Conduction System - drug effects</subject><subject>Heart Rate - drug effects</subject><subject>Humans</subject><subject>Infusions, Intravenous</subject><subject>Male</subject><subject>Medical sciences</subject><subject>Mibefradil - administration & dosage</subject><subject>Mibefradil - blood</subject><subject>Mibefradil - pharmacokinetics</subject><subject>Mibefradil - pharmacology</subject><subject>Pharmacology. Drug treatments</subject><subject>Reference Values</subject><issn>0009-9236</issn><issn>1532-6535</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2000</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNqFkLtPwzAQhy0EgvKY2VAGxJbii1vHhglVvKQKOpTZcq4OGJwHdirU_x5HqYCN6XT297vTfYScAh0D5fllhe04o7TvJhz4DhnBlGUpn7LpLhnFD5nKjPEDchjCe2wnUoh9cgA0nwDPxIhcPzW1s7XRPvmIpbMYEl2vkvZN-0pj45pXi4k3oW3qYJKuSSpbmNLrlXXHZK_ULpiTbT0iL3e3y9lDOn--f5zdzFNkUsgUygJ5XgoJIHIjDJaUwSpnU8qFzIECMmACTYaAsgCjJZWsZIWASJRYsCNyMcxtffO5NqFTlQ1onNO1adZB5VRKTrMsgpcDiL4JwZtStd5W2m8UUNX7UtGX6n2pwVdMnG1Hr4vKrP7wg6AInG8BHVC7eHiNNvxyjIEU_earAfuyzmz-W6tmi-Vsvlj2TyBjOBnCte7W3vyk0bXdFvkGAHiOvg</recordid><startdate>200003</startdate><enddate>200003</enddate><creator>Souich, Patrick</creator><creator>Besner, Jean‐Guy</creator><creator>Clozel, Jean‐Paul</creator><creator>Welker, Horst A.</creator><creator>Lefebvre, Marc</creator><creator>Caillé, Gilles</creator><general>Nature Publishing</general><scope>IQODW</scope><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope></search><sort><creationdate>200003</creationdate><title>Nonlinear kinetics and pharmacologic response to mibefradil</title><author>Souich, Patrick ; Besner, Jean‐Guy ; Clozel, Jean‐Paul ; Welker, Horst A. ; Lefebvre, Marc ; Caillé, Gilles</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-c3989-1fbc67f891187e8ecf031d73506897101c3138ce2c1c9b1ea9093f3b81506fcb3</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2000</creationdate><topic>Administration, Oral</topic><topic>Adult</topic><topic>Antihypertensive agents</topic><topic>Antihypertensive Agents - administration & dosage</topic><topic>Antihypertensive Agents - blood</topic><topic>Antihypertensive Agents - pharmacokinetics</topic><topic>Antihypertensive Agents - pharmacology</topic><topic>Biological and medical sciences</topic><topic>Biological Availability</topic><topic>Cardiovascular system</topic><topic>Drug Administration Schedule</topic><topic>Gas Chromatography-Mass Spectrometry</topic><topic>Heart Conduction System - drug effects</topic><topic>Heart Rate - drug effects</topic><topic>Humans</topic><topic>Infusions, Intravenous</topic><topic>Male</topic><topic>Medical sciences</topic><topic>Mibefradil - administration & dosage</topic><topic>Mibefradil - blood</topic><topic>Mibefradil - pharmacokinetics</topic><topic>Mibefradil - pharmacology</topic><topic>Pharmacology. Drug treatments</topic><topic>Reference Values</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Souich, Patrick</creatorcontrib><creatorcontrib>Besner, Jean‐Guy</creatorcontrib><creatorcontrib>Clozel, Jean‐Paul</creatorcontrib><creatorcontrib>Welker, Horst A.</creatorcontrib><creatorcontrib>Lefebvre, Marc</creatorcontrib><creatorcontrib>Caillé, Gilles</creatorcontrib><collection>Pascal-Francis</collection><collection>Medline</collection><collection>MEDLINE</collection><collection>MEDLINE (Ovid)</collection><collection>MEDLINE</collection><collection>MEDLINE</collection><collection>PubMed</collection><collection>CrossRef</collection><collection>MEDLINE - Academic</collection><jtitle>Clinical pharmacology and therapeutics</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Souich, Patrick</au><au>Besner, Jean‐Guy</au><au>Clozel, Jean‐Paul</au><au>Welker, Horst A.</au><au>Lefebvre, Marc</au><au>Caillé, Gilles</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Nonlinear kinetics and pharmacologic response to mibefradil</atitle><jtitle>Clinical pharmacology and therapeutics</jtitle><addtitle>Clin Pharmacol Ther</addtitle><date>2000-03</date><risdate>2000</risdate><volume>67</volume><issue>3</issue><spage>249</spage><epage>257</epage><pages>249-257</pages><issn>0009-9236</issn><eissn>1532-6535</eissn><coden>CLPTAT</coden><abstract>Background
Increasing oral doses of mibefradil (10 to 320 mg) decrease its apparent oral clearance; however, intravenous doses up to 80 mg do not reduce its systemic clearance. This study aimed to understand the mechanisms underlying the zero‐order kinetics of mibefradil.
Methods
A group of 10 normotensive volunteers received 50 mg/day oral mibefradil for 8 days and, on days 1 and 8, 5 mg deuterated mibefradil by infusion. Ten additional volunteers observed the same protocol with a daily oral dose of 100 mg mibefradil. Serial blood samples were withdrawn, and mibefradil plasma concentrations were assayed by liquid chromatography–mass spectrometry. Blood pressure and heart rate were measured for 4 hours, and an ECG was performed 2 hours after drug administration.
Results
Repeated oral administration of 50 mg mibefradil generated zero‐order kinetics secondary to a decrease in mibefradil systemic clearance. Compared with the 50‐mg dose, single and repeated oral doses of 100 mg further decreased mibefradil clearance. Mibefradil bioavailability was not affected by increasing mibefradil doses. Mean diastolic blood pressure was decreased by single and repeated doses of 100 mg to the same extent. Repeated doses of 100 mg reduced heart rate and prolonged the PR and QTc, changes that were associated with mibefradil plasma concentrations.
Conclusions
Repeated doses of 50 mg or doses of 100 mg mibefradil generated zero‐order kinetics secondary to a decrease in hepatic extraction of the drug. Zero‐order kinetics did not affect the response‐concentration relationship of mibefradil. (Clin Pharmacol Ther 2000;67:249–57.)
Clinical Pharmacology & Therapeutics (2000) 67, 249–257; doi: 10.1067/mcp.2000.104616</abstract><cop>New York, NY</cop><pub>Nature Publishing</pub><pmid>10741628</pmid><doi>10.1067/mcp.2000.104616</doi><tpages>9</tpages></addata></record> |
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| ispartof | Clinical pharmacology and therapeutics, 2000-03, Vol.67 (3), p.249-257 |
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| subjects | Administration, Oral Adult Antihypertensive agents Antihypertensive Agents - administration & dosage Antihypertensive Agents - blood Antihypertensive Agents - pharmacokinetics Antihypertensive Agents - pharmacology Biological and medical sciences Biological Availability Cardiovascular system Drug Administration Schedule Gas Chromatography-Mass Spectrometry Heart Conduction System - drug effects Heart Rate - drug effects Humans Infusions, Intravenous Male Medical sciences Mibefradil - administration & dosage Mibefradil - blood Mibefradil - pharmacokinetics Mibefradil - pharmacology Pharmacology. Drug treatments Reference Values |
| title | Nonlinear kinetics and pharmacologic response to mibefradil |
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