Literature DB >> 12839868

Despite increased plasma concentration, inflammation reduces potency of calcium channel antagonists due to lower binding to the rat heart.

Saeed Sattari1, William F Dryden, Lise A Eliot, Fakhreddin Jamali.   

Abstract

1. Rheumatoid arthritis reduces verapamil oral clearance thereby increases plasma concentration of the drug. This coincides with reduced drug effects through an unknown mechanism. 2. The effect of interferon-induced acute inflammation on the pharmacokinetics and electrocardiogram of verapamil (20 mg kg(-1), p.o.) and nifedipine (0.1 mg kg(-1), i.v.) was studied in Sprague-Dawley rats. 3. The effect of both acute and chronic inflammation on radioligand binding to cardiac L-type calcium channels was also investigated. 4. Acute inflammation resulted in increased plasma concentration of verapamil but had no effect on that of nifedipine. Verapamil binding to plasma proteins was unaffected. 5. As has been reported for humans, the increased verapamil concentration coincided with a reduction in the degree to which PR interval is prolonged by the drug. The effect of nifedipine on PR interval was also reduced by inflammation. 6. Maximum binding of (3)H-nitrendipine to cardiac cell membrane was significantly reduced from 63.2+/-2.5 fmol mg(-1) protein in controls to 46.4+/-2.0 in acute inflammation and from 66.8+/-2.2 fmol mg(-1) protein in controls to 42.2+/-2.0 in chronic inflammation. 7. Incubation of the normal cardiac cell membranes with 100 and 1000 pg ml(-1) of rat tissue necrosis factor-alpha did not influence the binding indices to the calcium channels. 8. Our data suggest that the reduced calcium channel responsiveness is because of altered binding to channels.

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Year:  2003        PMID: 12839868      PMCID: PMC1573909          DOI: 10.1038/sj.bjp.0705202

Source DB:  PubMed          Journal:  Br J Pharmacol        ISSN: 0007-1188            Impact factor:   8.739


  58 in total

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Journal:  Biochem Pharmacol       Date:  1986-05-01       Impact factor: 5.858

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Journal:  Arch Int Pharmacodyn Ther       Date:  1991 May-Jun

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Journal:  Br J Rheumatol       Date:  1984-05

Review 6.  Immunomodulating agents and hepatic drug-metabolizing enzymes.

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Journal:  Drug Metab Rev       Date:  1985       Impact factor: 4.518

7.  Increased plasma protein binding of propranolol and chlorpromazine mediated by disease-induced elevations of plasma alpha1 acid glycoprotein.

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Journal:  N Engl J Med       Date:  1978-12-28       Impact factor: 91.245

8.  Effect of altered plasma protein binding on pharmacokinetics and pharmacodynamics of propranolol in rats after surgery: role of alpha-1-acid glycoprotein.

Authors:  M Yasuhara; J Fujiwara; S Kitade; H Katayama; K Okumura; R Hori
Journal:  J Pharmacol Exp Ther       Date:  1985-11       Impact factor: 4.030

9.  Binding to serum alpha 1-acid glycoprotein and effect of beta-adrenoceptor antagonists in rats with inflammation.

Authors:  F M Belpaire; M G Bogaert; P Mugabo; M T Rosseel
Journal:  Br J Pharmacol       Date:  1986-07       Impact factor: 8.739

10.  Mechanism responsible for altered propranolol disposition in adjuvant-induced arthritis in the rat.

Authors:  K A Walker; H E Barber; G M Hawksworth
Journal:  Drug Metab Dispos       Date:  1986 Jul-Aug       Impact factor: 3.922

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5.  Effect of obesity on response to cardiovascular drugs in pediatric patients with renal disease.

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6.  Effects of angiotensin II blockade on inflammation-induced alterations of pharmacokinetics and pharmacodynamics of calcium channel blockers.

Authors:  S Hanafy; N J Dagenais; W F Dryden; F Jamali
Journal:  Br J Pharmacol       Date:  2007-10-29       Impact factor: 8.739

Review 7.  Interaction of local anesthetics with biomembranes consisting of phospholipids and cholesterol: mechanistic and clinical implications for anesthetic and cardiotoxic effects.

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8.  Local anesthetic failure associated with inflammation: verification of the acidosis mechanism and the hypothetic participation of inflammatory peroxynitrite.

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9.  Pharmacokinetic and Toxicodynamic Characterization of a Novel Doxorubicin Derivative.

Authors:  Samaa Alrushaid; Casey L Sayre; Jaime A Yáñez; M Laird Forrest; Sanjeewa N Senadheera; Frank J Burczynski; Raimar Löbenberg; Neal M Davies
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  9 in total

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