Literature DB >> 32038807

Assessment of General and Cardiac Toxicities of Astemizole in Male Cynomolgus Monkeys: Serum Biochemistry and Action Potential Duration.

Jong-Hwa Lee1, Do-Geun Kim1, Joung-Wook Seo2, Hyang-Ae Lee1, Jeong-Hwa Oh1, Ho-Chul Shin3, Seok Joo Yoon1, Choong-Yong Kim1.   

Abstract

Toxicology screening following treatment with astemizole, a histamine receptor antagonist, at oral doses of 0, 10, 30 and 60 mg/kg was carried out in male cynomolgus monkeys (Macaca fascicularis). No dose-related changes in mortality, clinical signs, body weight changes, food consumption, or urine analysis occurred in any animal compared to the vehicle control. However, the high-dose group showed a decrease in BUN and ALP compared to vehicle control group. In addition, the levels of TG, AST, ALP and CK increased. Although astemizole did not produce significant toxicological changes at any dose tested, we predict that it can cause toxicological changes of the liver and heart based on the changes in the serum parameters related to the heart and liver. The Action Potential Duration (APD) was prolonged in the heart of 60 mg/kg treatment group compared to the control group. The APD increase in 60 mg/kg treatment group along the other related changes in toxicological parameters imply that astemizole has major cardiotoxic effects in the cynomolgus monkey. This study is a valuable assessment for predicting the general toxicity and cardiotoxic effects of antihistamine drugs using nonhuman primates. © Korean Society of Toxicology 2008.

Entities:  

Keywords:  APD; Astemizole; Cardiotoxicity; Cynomolgus monkey; Serum biochemistry

Year:  2008        PMID: 32038807      PMCID: PMC7006242          DOI: 10.5487/TR.2008.24.4.289

Source DB:  PubMed          Journal:  Toxicol Res        ISSN: 1976-8257


  8 in total

1.  Reference values for clinical chemistry and clinical hematology parameters in cynomolgus monkeys.

Authors:  Henk-Jan Schuurman; Harold T Smith
Journal:  Xenotransplantation       Date:  2005-01       Impact factor: 3.907

2.  Chronic left atrial volume overload abbreviates the action potential duration of the canine pulmonary vein myocardium via activation of IK channel.

Authors:  Hideaki Nouchi; Akira Takahara; Hideki Nakamura; Iyuki Namekata; Takahiko Sugimoto; Yayoi Tsuneoka; Kiyoshi Takeda; Toshikazu Tanaka; Koki Shigenobu; Atsushi Sugiyama; Hikaru Tanaka
Journal:  Eur J Pharmacol       Date:  2008-09-10       Impact factor: 4.432

Review 3.  Clinical pathology reference ranges of laboratory animals. Working Group II, Nonclinical Safety Evaluation Subcommittee of the Japan Pharmaceutical Manufacturers Association.

Authors:  T Matsuzawa; M Nomura; T Unno
Journal:  J Vet Med Sci       Date:  1993-06       Impact factor: 1.267

4.  Torsade de pointes with an antihistamine metabolite: potassium channel blockade with desmethylastemizole.

Authors:  V R Vorperian; Z Zhou; S Mohammad; T J Hoon; C Studenik; C T January
Journal:  J Am Coll Cardiol       Date:  1996-11-15       Impact factor: 24.094

Review 5.  Torsades de pointes ventricular tachycardia associated with overdose of astemizole.

Authors:  K A Rao; A Adlakha; B Verma-Ansil; T D Meloy; M S Stanton
Journal:  Mayo Clin Proc       Date:  1994-06       Impact factor: 7.616

6.  Inhibition of the Na+/Ca2+ exchanger suppresses torsades de pointes in an intact heart model of long QT syndrome-2 and long QT syndrome-3.

Authors:  Peter Milberg; Christian Pott; Martin Fink; Gerrit Frommeyer; Toshio Matsuda; Akemichi Baba; Nani Osada; Günter Breithardt; Denis Noble; Lars Eckardt
Journal:  Heart Rhythm       Date:  2008-06-28       Impact factor: 6.343

Review 7.  Cardiotoxicity of new antihistamines and cisapride.

Authors:  Ilari Paakkari
Journal:  Toxicol Lett       Date:  2002-02-28       Impact factor: 4.372

8.  Reference range data base for serum chemistry and hematology values in laboratory animals.

Authors:  S T Wolford; R A Schroer; F X Gohs; P P Gallo; M Brodeck; H B Falk; R Ruhren
Journal:  J Toxicol Environ Health       Date:  1986
  8 in total

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