Literature DB >> 12603173

Clinical pharmacokinetics and pharmacodynamics of glyceryl trinitrate and its metabolites.

Satoru Hashimoto1, Atsuko Kobayashi.   

Abstract

This review discusses the pharmacokinetics and pharmacodynamics of glyceryl trinitrate (nitroglycerin; GTN) pertinent to clinical medicine. The pharmacokinetics of GTN associated with various dose regimens are characterised by prominent intra- and inter-individual variability. It is, nevertheless, important to clearly understand the pharmacokinetics and characteristics of GTN to optimise its use in clinical practice and, in particular, to obviate the development of tolerance. Measurements of plasma concentrations of GTN and of 1,2-glyceryl dinitrate (1,2-GDN), 1,3-glyceryl dinitrate (1,3-GDN), 1-glyceryl mononitrate (1-GMN), and 2-glyceryl mononitrate (2-GMN), its four main metabolites, remain difficult and require meticulous techniques to obtain reliable results. Since GDNs have an effect on haemodynamic function, pharmacokinetic analyses that include the parent drug as well as the metabolites are important. Although the precise mechanisms of GTN metabolism have not been elucidated, two main pathways have been proposed for its biotransformation. The first is a mechanism-based biotransformation pathway that produces nitric oxide (NO) and contributes directly to vasodilation. The second is a clearance-based biotransformation or detoxification pathway that produces inorganic nitrite anions (NO(2) -). NO(2) - has no apparent cardiovascular effect and is not converted to NO in pharmacologically relevant concentrations in vivo. In addition, several non-enzymatic and enzymatic systems are capable of metabolising GTN. This complex metabolism complicates considerably the evaluation of the pharmacokinetics and pharmacodynamics of GTN. Regardless of the route of administration, concentrations of the metabolites exceed those of the parent compound by several orders of magnitude. During continuous steady-state delivery of GTN, for instance by a patch, concentrations of 1,2-GDN are consistently 2-7 times higher than those of 1,3-GDN, and concentrations of 2-GMN are 4-8 times higher than those of 1-GMN. Concentrations of GDNs are approximately 10 times higher, and of GMNs approximately 100 times higher, than those of GTN during sustained administration. The development of tolerance is closely related to the metabolism of GTN, and can be broadly categorised as haemodynamic tolerance versus vascular tolerance. Efforts are warranted to circumvent the development of tolerance and facilitate the use of GTN in clinical practice. Although this remains to be accomplished, it is likely that, in the near future, regimens will be developed based on a full understanding of the pharmacokinetics and pharmacodynamics of GTN and its metabolites.

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Year:  2003        PMID: 12603173     DOI: 10.2165/00003088-200342030-00001

Source DB:  PubMed          Journal:  Clin Pharmacokinet        ISSN: 0312-5963            Impact factor:   6.447


  118 in total

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Journal:  Biochem Pharmacol       Date:  1993-10-19       Impact factor: 5.858

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  24 in total

1.  Sex differences in cardiovascular drug-induced adverse reactions causing hospital admissions.

Authors:  Eline M Rodenburg; Bruno H Stricker; Loes E Visser
Journal:  Br J Clin Pharmacol       Date:  2012-12       Impact factor: 4.335

2.  Constitutive nitric oxide synthase activation is a significant route for nitroglycerin-mediated vasodilation.

Authors:  Marcelo G Bonini; Krisztian Stadler; Sueli de Oliveira Silva; Jean Corbett; Michael Dore; John Petranka; Denise C Fernandes; Leonardo Y Tanaka; Danielle Duma; Francisco R M Laurindo; Ronald P Mason
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Authors:  Anu Shilpa Krishnatry; Sun Mi Fung; Daniel A Brazeau; David Soda; Ho-Leung Fung
Journal:  Nitric Oxide       Date:  2010-12-13       Impact factor: 4.427

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Authors:  Zhiqiang Chen; Matthew W Foster; Jian Zhang; Lan Mao; Howard A Rockman; Toshihiro Kawamoto; Kyoko Kitagawa; Keiichi I Nakayama; Douglas T Hess; Jonathan S Stamler
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5.  Nitroglycerin-induced S-nitrosylation and desensitization of soluble guanylyl cyclase contribute to nitrate tolerance.

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Journal:  Circ Res       Date:  2008-07-31       Impact factor: 17.367

6.  Systemic glyceryl trinitrate reduces anal sphincter tone: is there a therapeutic indication?

Authors:  C Connolly; S Tierney; P Grace
Journal:  Ir J Med Sci       Date:  2017-09-13       Impact factor: 1.568

7.  Does the use of ketamine or nitroglycerin as an adjuvant to lidocaine improve the quality of intravenous regional anesthesia?

Authors:  Khaled Fawzy Elmetwaly; Nasr Abdelmohsen Hegazy; Abdelkhalek Abdelmonem Aboelseoud; Ahmad Abdullah Alshaer
Journal:  Saudi J Anaesth       Date:  2010-05

8.  Protein disulfide-isomerase interacts with soluble guanylyl cyclase via a redox-based mechanism and modulates its activity.

Authors:  Erin J Heckler; Pierre-Antoine Crassous; Padmamalini Baskaran; Annie Beuve
Journal:  Biochem J       Date:  2013-05-15       Impact factor: 3.857

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Authors:  D Dou; X Zheng; X Qin; H Qi; L Liu; J U Raj; Y Gao
Journal:  Br J Pharmacol       Date:  2007-11-26       Impact factor: 8.739

Review 10.  0.4% nitroglycerin ointment : in the treatment of chronic anal fissure pain.

Authors:  Caroline Fenton; Keri Wellington; Stephanie E Easthope
Journal:  Drugs       Date:  2006       Impact factor: 9.546

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