The effect of thalidomide and supidimide on endotoxin-induced uveitis in rats |
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Authors: | Yan Guex-Crosier N Pittet C P Herbort |
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Institution: | (1) Hôpital Jules Gonin, Department of Ophthalmology, University of Lausanne, 15 Av. de France, CH-1004 Lausanne, Switzerland;(2) Present address: National Institutes of Health, National Eye Institute, Bldg. 10, Room 10 N 112, 9000 Rockville Pike, 20892 Bethesda, MD, USA;(3) Present address: Eye Center La Source , 2 Av. des Bergières, CH-1004 Lausanne, Switzerland |
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Abstract: | Background: Endotoxin-induced uveitis (EIU) is an animal model of ocular inflammation, produced by footpad injection of endotoxin (lipopolysaccharide, LPS) to mimic the human disease of acute anterior uveitis, that is useful for testing new anti-inflammatory therapy. The purpose of this study was to test the anti-inflammatory effect on EIU of thalidomide and one of its derivatives, supidimide. Methods: EIU was produced in rats by hind footpad injection of LPS (100 g/animal). Animals were killed 20 h after LPS injection. Inflammation was evaluated by anterior chamber determination of proteins and cells. Results: A dosage of 400 mg/kg per day of thalidomide was efficient in reducing inflammation whether given in three doses (at – 24 h, – 4 h and + 4 h relative to LPS challenge = THAL-1; p < 0.001 for proteins and cells), in two doses (–4 h and +4 h = THAL-2; p < 0.001 for proteins, p < 0.012 for cells) or in one dose (at +4 h=late THAL; p < 0.001 for proteins, p 0.02 for cells). A dosage of 300 mg/kg per day of thalidomide was still efficient (p 0.023 for proteins, p 0.06 for cells), but 150 mg/kg per day had no effect on inflammation. Supidimide (400 mg/kg per day) had some anti-inflammatory effect (p 0.053 for proteins, p < 0.06 for cells). Conclusion: High-dose thalidomide had a potent anti-inflammatory effect in EIU, but lower doses were not sufficient to reduce inflammation. At similar high doses, supidimide had some effect on EIU but was less effective than thalidomide.These data were presented in part at the first annual ECORA meeting, 4–6 October, 1993, Bonn, Germany |
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