Top 2 papers published by Jürgen M. Lehmann from Research Triangle Park in 2003

Patent•

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Curt Dale Haffner, Patrick Reed Maloney, Timothy M. Willson, Steven G. Blanchard, Steven A. Kliewer, Jürgen M. Lehmann, Derek J. Parks, Julie B. Stimmel - Show less +4 more

08 Aug 2003

TL;DR: In this paper, a method for identifying ligands for nuclear receptors, utilizing scintillation proximity and fluorescence resonance energy transfer (FRET), and methods of using identified ligands.

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Abstract: The present invention includes nuclear receptor heterodimer and nuclear receptor-coactivator peptide assays for identifying ligands for nuclear receptors, utilizing scintillation proximity and fluorescence resonance energy transfer (FRET), and methods of using identified ligands.

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11 citations

Journal Article•DOI•

CYP3A induction by N-hydroxyformamide tumor necrosis factor-α converting enzyme/matrix metalloproteinase inhibitors: Use of a pregnane X receptor activation assay and primary hepatocyte culture for assessing induction potential in humans

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Timothy K. Tippin¹, G. Hamilton², Linda B. Moore³, Elizabeth J. Beaudet³, Summer Jolley², Thomas A. Brodie³, Andrews Robert Carl³, J. David Becherer³, Darryl L. McDougald³, Michael D. Gaul³, Debie J. Hoivik³, Kathy Mellon-Kusibab³, Jürgen M. Lehmann³, Steven A. Kliewer³, Steven J. Novick³, Ron Laethem³, Zhiyang Zhao³, Edward L. LeCluyse² - Show less +14 more•Institutions (3)

Research Triangle Park¹, University of North Carolina at Chapel Hill², GlaxoSmithKline³

01 Jul 2003-Drug Metabolism and Disposition

TL;DR: The extent of rodent CYP3A induction caused by GW3333 was confirmed in vivo after daily oral administration for 14 days to rats, and other N-hydroxyformamides are less likely to induce CYP 3A.

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Abstract: A series of N-hydroxyformamide tumor necrosis factor- converting enzyme (TACE)/matrix metalloprotease (MMP) inhibitors were evaluated for their potential to induce human cytochrome P450 3A (CYP3A). Two in vitro assays were used: 1) a cell-based reporter gene assay for activation of the pregnane X receptor (PXR), and 2) a primary “sandwich” culture of human hepatocytes. Approximately 50 TACE/MMP inhibitors were evaluated in the human PXR assay. A range of PXR activation was observed, 0 to 150% of the activation of the known human CYP3A inducer rifampicin. Three TACE/MMP inhibitors were evaluated in rat and human hepatocytes. Significantly higher PXR activation/CYP3A induction was observed in PXR/hepatocyte models, respectively, for (2R,3S) 3-(formyl-hydroxyamino)-2(2-methyl-1-propyl)-4-methylpentanoic acid [(1S,2S)-2-methyl-1-(2pyridylcarbamoyl)-1-butyl]amide (GW3333) compared with (2R,3S)6,6,6-trifluoro-3-[formyl(hydroxy)amino]-2-isobutyl-N-{(1S,2R)-2methoxy-1-[(1,3-thiazol-2-ylamino)carbonyl]propyl}hexanamide (GW6495) and (2R)-N-{(1S)-2,2-dimethyl-1-[(methylamino)carbonyl]propyl}-2-{(1S)-1-[formyl(hydroxy)amino]ethyl}-5-phenylpentanamide (GI4023). The CYP3A induction level achieved with GW3333 at a concentration of approximately 10 M in human hepatocytes was comparable to that achieved with rifampicin at a concentration of 10 M. The extent of rodent CYP3A induction caused by GW3333 was confirmed in vivo after daily oral administration for 14 days to rats. In conclusion, GW3333 is a potential inducer of CYP3A expression in vivo in humans, but other N-hydroxyformamides are less likely to induce CYP3A.

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10 citations

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