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Current status of safety and efficacy of calcium channel blockers in cardiovascular diseases: A critical analysis based on 100 studies

Identifieur interne : 002A08 ( Istex/Corpus ); précédent : 002A07; suivant : 002A09

Current status of safety and efficacy of calcium channel blockers in cardiovascular diseases: A critical analysis based on 100 studies

Auteurs : Lionel H. Opie ; Salim Yusuf ; Wolfgang Kübler

Source :

RBID : ISTEX:14D424F49DCF98802C7A833DA9B2844D2FE8FBE3

Abstract

Recently, serious concerns have been expressed about the long-term safety of the calcium channel blockers (CCBs) as a group. Safety and efficacy are, however, ultimately linked to each other; therefore both must be evaluated especially in the therapy of angina and hypertension, the main clinical indications for CCBs. The structural, functional, and pharmacokinetic heterogeneity of CCBs means that the efficacy and dangers of one subclass, such as the short-acting dihydropyridines (DHPs), in one situation, such as unstable angina, do not necessarily apply in other clinical situations. One hundred studies are reviewed according to their methods of data collection: case series, case control, cohort, randomized controlled trials (RCTs), and meta-analyses. Large, well-designed RCTs and the meta-analyses based on these trials remain the gold standard. Observational studies, though potentially less reliable sources of information because of selection bias, may nevertheless produce hypotheses that must then be tested in RCTs. Regarding safety, both observational studies and RCTs suggest that adverse effects of CCBs may be linked to short-acting agents, specifically short-acting nifedipine. Two good studies favor the safety of verapamil, even in short-acting form. Incomplete but increasing overall evidence favors the safety of longer-acting DHPs. Heart failure remains a class contraindication to the use of all CCBs, with some exceptions. Regarding efficacy, there are positive results of RCTs with CCBs in 2 specific clinical situations, namely, verapamil in postinfarct protection in the absence of pre-existing heart failure, and 2 outcome studies on hypertension with longer acting DHPs. These results cannot automatically be applied to other clinical situations and to other CCBs. For example, there is no evidence for the safety or efficacy of DHPs used without β blockers in postinfarct patients. In diabetic hypertensives, 2 relatively large RCTs show that the blood pressure can be reduced by DHP-based therapy in diabetics, with a reduction in hard end points. To achieve current blood pressure goals, combination therapy is almost always necessary, and in diabetics there is strong evidence that 1 essential component should be an angiotensin converting enzyme inhibitor. The future aim with CCBs must be to obtain a large database gathered from RCTs, which will give the same certainty about efficacy and safety that already holds for use of the diuretics in hypertension, β-blockers in postmyocardial infarction patients, and the angiotensin converting enzyme inhibitors in heart failure. Copyright © 2000 by W.B. Saunders Company Progress in Cardiovascular Diseases, Vol. 43, No. 2 (September/October), 2000: pp 171-196

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DOI: 10.1053/pcad.2000.7010

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<note type="content">TABLE 1: Binding Sites for Calcium Channel Antagonists, Tissue Specificity, Clinical Uses, and Safety Concerns</note>
<note type="content">TABLE 2: Current Evidence on Safety and Efficacy of CCBs in Ischemic Heart Disease and Hypertension</note>
<note type="content">TABLE 3: Hazards of Database Analyses in Evaluating the Efficacy of Therapy</note>
<note type="content">TABLE 4: Randomized Control Trials of CCBs in Effort or Unstable Angina</note>
<note type="content">TABLE 5: Randomized Controlled Trials in Early MI and Post-MI: Key Trials With CCBs</note>
<note type="content">TABLE 6: Outcome Studies in Vascular Disease Studies With CCBs</note>
<note type="content">TABLE 7: Case Control or Cohort Studies: Risk of AMI or Total Cardiovascular Risk in Hypertensives Treated by CCBs</note>
<note type="content">TABLE 8: Controlled Outcome Trials of CCBs in Hypertension</note>
<note type="content">TABLE 9: Recent Randomized Controlled Outcome Trials of CCBs in Heart Failure</note>
<note type="content">TABLE 10: Nonrandomized Cohort Studies: Risk of Mortality With CCB Therapy</note>
<note type="content">TABLE 11: Risk of Cancer With CCBs in Major Studies</note>
<note type="content">TABLE 12: Does Use of CCBs Predispose to Bleeding?</note>
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<ce:simple-para>Recently, serious concerns have been expressed about the long-term safety of the calcium channel blockers (CCBs) as a group. Safety and efficacy are, however, ultimately linked to each other; therefore both must be evaluated especially in the therapy of angina and hypertension, the main clinical indications for CCBs. The structural, functional, and pharmacokinetic heterogeneity of CCBs means that the efficacy and dangers of one subclass, such as the short-acting dihydropyridines (DHPs), in one situation, such as unstable angina, do not necessarily apply in other clinical situations. One hundred studies are reviewed according to their methods of data collection: case series, case control, cohort, randomized controlled trials (RCTs), and meta-analyses. Large, well-designed RCTs and the meta-analyses based on these trials remain the gold standard. Observational studies, though potentially less reliable sources of information because of selection bias, may nevertheless produce hypotheses that must then be tested in RCTs. Regarding safety, both observational studies and RCTs suggest that adverse effects of CCBs may be linked to short-acting agents, specifically short-acting nifedipine. Two good studies favor the safety of verapamil, even in short-acting form. Incomplete but increasing overall evidence favors the safety of longer-acting DHPs. Heart failure remains a class contraindication to the use of all CCBs, with some exceptions. Regarding efficacy, there are positive results of RCTs with CCBs in 2 specific clinical situations, namely, verapamil in postinfarct protection in the absence of pre-existing heart failure, and 2 outcome studies on hypertension with longer acting DHPs. These results cannot automatically be applied to other clinical situations and to other CCBs. For example, there is no evidence for the safety or efficacy of DHPs used without β blockers in postinfarct patients. In diabetic hypertensives, 2 relatively large RCTs show that the blood pressure can be reduced by DHP-based therapy in diabetics, with a reduction in hard end points. To achieve current blood pressure goals, combination therapy is almost always necessary, and in diabetics there is strong evidence that 1 essential component should be an angiotensin converting enzyme inhibitor. The future aim with CCBs must be to obtain a large database gathered from RCTs, which will give the same certainty about efficacy and safety that already holds for use of the diuretics in hypertension, β-blockers in postmyocardial infarction patients, and the angiotensin converting enzyme inhibitors in heart failure. Copyright © 2000 by W.B. Saunders Company</ce:simple-para>
<ce:simple-para>
<ce:italic>Progress in Cardiovascular Diseases</ce:italic>
, Vol. 43, No. 2 (September/October), 2000: pp 171-196</ce:simple-para>
</ce:abstract-sec>
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<title>Current status of safety and efficacy of calcium channel blockers in cardiovascular diseases: A critical analysis based on 100 studies</title>
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<title>Current status of safety and efficacy of calcium channel blockers in cardiovascular diseases: A critical analysis based on 100 studies</title>
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<name type="personal">
<namePart type="given">Lionel H</namePart>
<namePart type="family">Opie</namePart>
<affiliation>University of Cape Town, Cape-Town, South Africa; the Department of Medicine, Division of Cardiology, McMaster University, Ontario, Canada; and the Department of Cardiology, University of Heidelberg, Heidelberg, Germany</affiliation>
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<namePart type="given">Salim</namePart>
<namePart type="family">Yusuf</namePart>
<affiliation>University of Cape Town, Cape-Town, South Africa; the Department of Medicine, Division of Cardiology, McMaster University, Ontario, Canada; and the Department of Cardiology, University of Heidelberg, Heidelberg, Germany</affiliation>
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<name type="personal">
<namePart type="given">Wolfgang</namePart>
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<affiliation>University of Cape Town, Cape-Town, South Africa; the Department of Medicine, Division of Cardiology, McMaster University, Ontario, Canada; and the Department of Cardiology, University of Heidelberg, Heidelberg, Germany</affiliation>
<affiliation>E-mail: Opie@samiot.uct.ac.za</affiliation>
<description>Address reprint requests to Lionel H. Opie, MD, DPhil, FRCP, Heart Research Unit, Cape Heart Centre, University of Cape Town Medical School, Observatory 7925, Cape Town, South Africa;</description>
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<abstract lang="en">Recently, serious concerns have been expressed about the long-term safety of the calcium channel blockers (CCBs) as a group. Safety and efficacy are, however, ultimately linked to each other; therefore both must be evaluated especially in the therapy of angina and hypertension, the main clinical indications for CCBs. The structural, functional, and pharmacokinetic heterogeneity of CCBs means that the efficacy and dangers of one subclass, such as the short-acting dihydropyridines (DHPs), in one situation, such as unstable angina, do not necessarily apply in other clinical situations. One hundred studies are reviewed according to their methods of data collection: case series, case control, cohort, randomized controlled trials (RCTs), and meta-analyses. Large, well-designed RCTs and the meta-analyses based on these trials remain the gold standard. Observational studies, though potentially less reliable sources of information because of selection bias, may nevertheless produce hypotheses that must then be tested in RCTs. Regarding safety, both observational studies and RCTs suggest that adverse effects of CCBs may be linked to short-acting agents, specifically short-acting nifedipine. Two good studies favor the safety of verapamil, even in short-acting form. Incomplete but increasing overall evidence favors the safety of longer-acting DHPs. Heart failure remains a class contraindication to the use of all CCBs, with some exceptions. Regarding efficacy, there are positive results of RCTs with CCBs in 2 specific clinical situations, namely, verapamil in postinfarct protection in the absence of pre-existing heart failure, and 2 outcome studies on hypertension with longer acting DHPs. These results cannot automatically be applied to other clinical situations and to other CCBs. For example, there is no evidence for the safety or efficacy of DHPs used without β blockers in postinfarct patients. In diabetic hypertensives, 2 relatively large RCTs show that the blood pressure can be reduced by DHP-based therapy in diabetics, with a reduction in hard end points. To achieve current blood pressure goals, combination therapy is almost always necessary, and in diabetics there is strong evidence that 1 essential component should be an angiotensin converting enzyme inhibitor. The future aim with CCBs must be to obtain a large database gathered from RCTs, which will give the same certainty about efficacy and safety that already holds for use of the diuretics in hypertension, β-blockers in postmyocardial infarction patients, and the angiotensin converting enzyme inhibitors in heart failure. Copyright © 2000 by W.B. Saunders Company Progress in Cardiovascular Diseases, Vol. 43, No. 2 (September/October), 2000: pp 171-196</abstract>
<note>0033-0620/00/4206-0004$10.00/0</note>
<note type="content">TABLE 1: Binding Sites for Calcium Channel Antagonists, Tissue Specificity, Clinical Uses, and Safety Concerns</note>
<note type="content">TABLE 2: Current Evidence on Safety and Efficacy of CCBs in Ischemic Heart Disease and Hypertension</note>
<note type="content">TABLE 3: Hazards of Database Analyses in Evaluating the Efficacy of Therapy</note>
<note type="content">TABLE 4: Randomized Control Trials of CCBs in Effort or Unstable Angina</note>
<note type="content">TABLE 5: Randomized Controlled Trials in Early MI and Post-MI: Key Trials With CCBs</note>
<note type="content">TABLE 6: Outcome Studies in Vascular Disease Studies With CCBs</note>
<note type="content">TABLE 7: Case Control or Cohort Studies: Risk of AMI or Total Cardiovascular Risk in Hypertensives Treated by CCBs</note>
<note type="content">TABLE 8: Controlled Outcome Trials of CCBs in Hypertension</note>
<note type="content">TABLE 9: Recent Randomized Controlled Outcome Trials of CCBs in Heart Failure</note>
<note type="content">TABLE 10: Nonrandomized Cohort Studies: Risk of Mortality With CCB Therapy</note>
<note type="content">TABLE 11: Risk of Cancer With CCBs in Major Studies</note>
<note type="content">TABLE 12: Does Use of CCBs Predispose to Bleeding?</note>
<subject>
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<topic>Special Articles</topic>
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<dateIssued encoding="w3cdtf">200010</dateIssued>
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<identifier type="ISSN">0033-0620</identifier>
<identifier type="PII">S0033-0620(00)X0006-0</identifier>
<part>
<date>200010</date>
<detail type="issue">
<title>Cerebrovascular Disease: Part II</title>
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<detail type="volume">
<number>43</number>
<caption>vol.</caption>
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<detail type="issue">
<number>2</number>
<caption>no.</caption>
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<start>101</start>
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<identifier type="DOI">10.1053/pcad.2000.7010</identifier>
<identifier type="PII">S0033-0620(00)00010-4</identifier>
<accessCondition type="use and reproduction" contentType="copyright">©2000 W.B. Saunders Company</accessCondition>
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