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Research ArticleArticle

Pharmacokinetics of Meloxicam in Animals and The Relevance to Humans

Ulrich Busch, Jochen Schmid, Günther Heinzel, Helmut Schmaus, Jürgen Baierl, Claudia Huber and Willy Roth
Drug Metabolism and Disposition June 1998, 26 (6) 576-584;
Ulrich Busch
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Jochen Schmid
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Günther Heinzel
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Helmut Schmaus
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Jürgen Baierl
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Claudia Huber
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Willy Roth
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Abstract

The pharmacokinetic profile of the new nonsteroidal anti-inflammatory drug meloxicam was investigated in a number of animal species, including mice, rats, dogs, mini-pigs, and baboons, after administration of [14C]meloxicam. The plasma concentration-time profiles for meloxicam in rats and dogs were comparable to that in humans, whereas there were marked differences between humans and mice, mini-pigs, and baboons. The highest tissue concentrations of meloxicam in rats and mini-pigs were seen in the liver and kidneys. In contrast, low concentrations of meloxicam were found in the central nervous system, compared with those in plasma. The excretion balance in mini-pigs resembled that in humans, with almost equal concentrations being eliminated in the urine and the feces. As in humans, meloxicam circulated mainly in the form of the parent compound in the plasma of mice, rats, dogs, mini-pigs, and baboons. The main metabolites in rats, mini-pigs, and humans were a 5′-hydroxymethyl derivative (AF-UH 1 SE) and a 5′-carboxy metabolite (UH-AC 110 SE). The percentage of meloxicam binding to protein was higher in rats and humans (>99%) than in other species. The pharmacokinetic profile of meloxicam in rats most closely resembles that in humans; therefore, reliable clinical predictions can be made from studies in this rodent species.

Footnotes

  • Send reprint requests to: Dr. Ulrich Busch, Boehringer Ingelheim Pharma KG, Birkendorfer Straβe 65, D-88397 Biberach an der Riss, Germany.

  • Abbreviations used are::
    NSAID
    nonsteroidal anti-inflammatory drug
    CL
    clearance of drug from plasma
    Cmax
    maximum concentration of drug in plasma
    F
    bioavailability factor
    id
    intraduodenal
    MRT
    mean residence time
    Vss
    apparent volume of distribution under steady-state conditions
    tmax
    time to reach the maximum concentration of drug in plasma
    Vz
    apparent volume of distribution during the terminalλz phase
    λz
    terminal elimination rate constant
    Vss
    apparent volume of distribution under steady-state conditions
    CYP
    cytochrome P450
    • Received June 20, 1997.
    • Accepted February 9, 1998.
  • The American Society for Pharmacology and Experimental Therapeutics
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Drug Metabolism and Disposition
Vol. 26, Issue 6
1 Jun 1998
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Research ArticleArticle

Pharmacokinetics of Meloxicam in Animals and The Relevance to Humans

Ulrich Busch, Jochen Schmid, Günther Heinzel, Helmut Schmaus, Jürgen Baierl, Claudia Huber and Willy Roth
Drug Metabolism and Disposition June 1, 1998, 26 (6) 576-584;

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Research ArticleArticle

Pharmacokinetics of Meloxicam in Animals and The Relevance to Humans

Ulrich Busch, Jochen Schmid, Günther Heinzel, Helmut Schmaus, Jürgen Baierl, Claudia Huber and Willy Roth
Drug Metabolism and Disposition June 1, 1998, 26 (6) 576-584;
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