Abstract
Neurotoxicity, a crucial side effect of immunosuppressive therapy with cyclosporine, also has been demonstrated in vitro for sirolimus, a novel macrolide immunosuppressant, which is under clinical investigation in combination with cyclosporine. NMR spectroscopy was used to study the separate and combined effects of cyclosporine and sirolimus on cerebral metabolism, both in brain cells and in perfused rat brain slices. The high-energy phosphate metabolism was already affected significantly at cyclosporine concentrations as low as 100 μg/liter: phosphocreatine was reduced by 10 ± 2% [half-maximal inhibition concentration (IC50) = 1850 ± 600 μg/liter], and nucleoside triphosphate was reduced by 11 ± 5% (IC50 = 1110 ± 420 μg/liter;n = 4, P < .05). At 500 μg/liter cyclosporine, N-acetylaspartate and glutamate were decreased by 13 ± 7% (IC50 = 1100 ± 330 μg/liter) and 22 ± 9% (IC50 = 360 ± 220 μg/liter; n = 4, P < .05), respectively. As evaluated using an algorithm based on Loewe isobolograms, combination of cyclosporine and sirolimus resulted in a synergetic reduction of high-energy phosphate metabolites. Addition of sirolimus to the perfusion medium increased brain slice concentrations of cyclosporine. It is concluded that cyclosporine significantly reduced high-energy phosphate metabolism in brain tissue at in vivo relevant concentrations. Combination with sirolimus resulted in synergism, which, in part, is explained by a greater distribution of cyclosporine into the brain tissue in the presence of sirolimus.
Footnotes
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Send reprint requests to: Uwe Christians, Department of Biopharmaceutical Sciences, School of Pharmacy, University of California at San Francisco, 513 Parnassus Ave., Room S-834, San Francisco, CA 94143. E-mail: uwec{at}itsa.ucsf.edu
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↵1 This study was supported by Alexander von Humboldt-Foundation Grant V-3-FLF-1052812 and Deutsche Forschungsgemeinschaft Grant Ch95/6–1.
- Abbreviations:
- IC50
- half-maximal inhibition concentration
- NAA
- N-acetylaspartate, NTP, nucleoside triphosphate
- PCA
- perchloric acid
- PCr
- phosphocreatine
- PME
- phosphomonoester
- TCA
- trichloroacetic acid
- MS
- mass spectroscopy
- Received June 8, 1998.
- Accepted December 1, 1998.
- The American Society for Pharmacology and Experimental Therapeutics
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