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Structure-intestinal transport and structure-metabolism correlations of some potential cancerostatic pyrimidine nucleosides in isolated rat jejunum
Authors:Ladislav Novotný  Hassan Farghali  Miloš Ryba  Ivo Janků  Jiří Beránek
Affiliation:(1) Institute of Organic Chemistry and Biochemistry, Czechoslovak Academy of Sciences, Fleming Sq. 2, 16610 Prague 6, Czechoslovakia;(2) Institute of Pharmacology, Czechoslovak Academy of Sciences, Fleming Sq. 2, 16610 Prague 6, Czechoslovakia
Abstract:Summary Both transport and biotransformation processes for a series of pyrimidine nucleobases, ribonucleosides, 2prime-deoxyribonucleosides, and acetyl and 5prime-substituted derivatives of the cancerostatic agent araC were studied in the isolated everted rat jejunum with a continuous perfusion technique. Metabolic alterations during penetration were assessed by HPLC. 5prime-Halogeno and 5prime-deoxy derivatives of cytosine nucleosides exhibited higher transport rates and higher stability towards the deamination reaction than did unsubstituted derivatives. Octanol-buffer partition coefficients were estimated for the study compounds, and fragmental constants for the sugar moieties of nucleosides were assessed. With the present study compounds there was no correlation between lipophilicity and transport rate, as previously reported, but there was a correlation between lipophilicity and metabolic alteration of araC derivatives (r=0.99, n=5).
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