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Research ArticleArticle

The Absorption, Metabolism, and Excretion of the Novel Neuromodulator RWJ-333369 (1,2-Ethanediol, [1-2-Chlorophenyl]-, 2-carbamate, [S]-) in Humans

G. S. J. Mannens, J. Hendrickx, C. G. M. Janssen, S. Chien, B. Van Hoof, T. Verhaeghe, M. Kao, M. F. Kelley, I. Goris, M. Bockx, B. Verreet, M. Bialer and W. Meuldermans
Drug Metabolism and Disposition April 2007, 35 (4) 554-565; DOI: https://doi.org/10.1124/dmd.106.011940
G. S. J. Mannens
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J. Hendrickx
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C. G. M. Janssen
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S. Chien
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B. Van Hoof
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T. Verhaeghe
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M. Kao
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M. F. Kelley
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I. Goris
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M. Bockx
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B. Verreet
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M. Bialer
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Abstract

RWJ-333369 (1,2-ethanediol, [1-2-chlorophenyl]-, 2-carbamate, [S]-; CAS Registry Number 194085-75-1) is a novel neuromodulator in clinical development for the treatment of epilepsy. To study the disposition of RWJ-333369, eight healthy male subjects received a single oral dose of 500 mg of 14C-RWJ-333369. Urine, feces, and plasma were collected for analysis for up to 1 week after dosing. Radioactivity was mainly excreted in urine (93.8 ± 6.6%) and much less in feces (2.5 ± 1.6%). RWJ-333369 was extensively metabolized in humans, since only low amounts of parent drug were excreted in urine (1.7% on average) and feces (trace amounts). The major biotransformation pathways were direct O-glucuronidation (44% of the dose), and hydrolysis of the carbamate ester followed by oxidation to 2-chloromandelic acid, which was subsequently metabolized in parallel to 2-chlorophenyl glycine and 2-chlorobenzoic acid (mean percentage of the dose for the three acids together was 36%). Other routes were chiral inversion followed by O-glucuronidation (11%), and aromatic hydroxylation in combination with sulfate conjugation (5%). In plasma, unchanged drug accounted for 76.5% of the total radioactivity, with the R-enantiomer and the O-glucuronide of the parent drug as the only measurable plasma metabolites. With the use of very sensitive liquid chromatography-tandem mass spectrometry techniques, only traces of aromatic (pre)mercapturic acid conjugates were detected in urine (each <0.3% of the dose), suggesting a low potential for reactive metabolite formation. In conclusion, the disposition of RWJ-333369 in humans is characterized by virtually complete absorption, extensive metabolism, and unchanged drug as the only significant circulating species.

Footnotes

  • Article, publication date, and citation information can be found at http://dmd.aspetjournals.org.

  • doi:10.1124/dmd.106.011940.

  • ABBREVIATIONS: HPLC, high-performance liquid chromatography; LC-MS/MS, liquid chromatography-tandem mass spectrometry; TR, total radioactivity; radio-HPLC, HPLC with radioactivity detection; ESI, electrospray ionization; UD, unchanged drug; MS, mass spectrometry; ATPAL, atropaldehyde; R293792, 2-(2-chlorophenyl)-2-(1,1-2H2-1,2-13C2)-hydroxyethyl carbamate; RWJ-452399, 1,2-ethanediol, [1-2-chlorophenyl]-, 2-carbamate, [R]-; JNJ-26642083, N-acetyl-S-(3-{(1S)-2-[aminocarbonyl)oxy]-1-hydroxyethyl}-4-chlorophenyl)-l-cysteine; JNJ-26954213, N-acetyl-S-(4-{(1S)-2-[aminocarbonyl)oxy]-1-hydroxyethyl}-3-chlorophenyl)-l-cysteine.

    • Received July 13, 2006.
    • Accepted August 24, 2006.
  • The American Society for Pharmacology and Experimental Therapeutics
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Drug Metabolism and Disposition: 35 (4)
Drug Metabolism and Disposition
Vol. 35, Issue 4
1 Apr 2007
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Research ArticleArticle

The Absorption, Metabolism, and Excretion of the Novel Neuromodulator RWJ-333369 (1,2-Ethanediol, [1-2-Chlorophenyl]-, 2-carbamate, [S]-) in Humans

G. S. J. Mannens, J. Hendrickx, C. G. M. Janssen, S. Chien, B. Van Hoof, T. Verhaeghe, M. Kao, M. F. Kelley, I. Goris, M. Bockx, B. Verreet, M. Bialer and W. Meuldermans
Drug Metabolism and Disposition April 1, 2007, 35 (4) 554-565; DOI: https://doi.org/10.1124/dmd.106.011940

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Research ArticleArticle

The Absorption, Metabolism, and Excretion of the Novel Neuromodulator RWJ-333369 (1,2-Ethanediol, [1-2-Chlorophenyl]-, 2-carbamate, [S]-) in Humans

G. S. J. Mannens, J. Hendrickx, C. G. M. Janssen, S. Chien, B. Van Hoof, T. Verhaeghe, M. Kao, M. F. Kelley, I. Goris, M. Bockx, B. Verreet, M. Bialer and W. Meuldermans
Drug Metabolism and Disposition April 1, 2007, 35 (4) 554-565; DOI: https://doi.org/10.1124/dmd.106.011940
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