The pharmacokinetics of prednimustine and chlorambucil in the rat

In the rat prednimustine, the prednisolone ester of chlorambucil, is much less toxic than equimolar doses of chlorambucil, when administered subcutaneously (SC). This is due to differences in alkylating agent pharmacokinetics. Prednimustine injected SC produced low plasma concentrations (less than 5...

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Bibliographic Details
Published in:Cancer chemotherapy and pharmacology 1981-01, Vol.6 (1), p.85
Main Authors: Newell, D R, Shepherd, C R, Harrap, K R
Format: Article
Language:English
Subjects:
Animals
Chlorambucil - analogs & derivatives
Chlorambucil - metabolism
Chlorambucil - therapeutic use
Chlorambucil - toxicity
Female
Kinetics
Prednimustine - metabolism
Prednimustine - therapeutic use
Prednimustine - toxicity
Rats
Rats, Inbred Strains
Sarcoma, Yoshida - drug therapy
Tissue Distribution
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Summary:In the rat prednimustine, the prednisolone ester of chlorambucil, is much less toxic than equimolar doses of chlorambucil, when administered subcutaneously (SC). This is due to differences in alkylating agent pharmacokinetics. Prednimustine injected SC produced low plasma concentrations (less than 5 microM) of the alkylating metabolites chlorambucil and phenyl acetic mustard, which were maintained for 48 h. No unhydrolysed prednimustine could be detected. Chlorambucil, in contrast, was rapidly absorbed, peak levels (40 microM) occurring within 2 h, after which chlorambucil and phenyl acetic mustard plasma levels decreased with half-lives of 2.4 h and 2.9 h respectively. The toxicity of chlorambucil could be similarly reduced by administering either the methyl ester of chlorambucil or by giving chlorambucil in a multiple-treatment low-dose schedule. Neither of these treatments inhibited the Yoshida alkylating agent-resistant tumour, however, whereas prednimustine or a combination of chlorambucil and prednisolone produced significant tumour growth inhibition. Prednisolone did not alter chlorambucil pharmacokinetics. Thus the reduced toxicity of prednimustine is due to chlorambucil esterification and the subsequent alteration in pharmacokinetics, whilst inhibition of alkylating agent-resistant tumours results from the combination of chlorambucil and prednisolone.
ISSN:0344-5704
1432-0843
DOI:10.1007/BF00253015