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Clinical Trial
. 1990;26(6):429-36.
doi: 10.1007/BF02994094.

Characterisation of urinary metabolites of temozolomide in humans and mice and evaluation of their cytotoxicity

Affiliations
Clinical Trial

Characterisation of urinary metabolites of temozolomide in humans and mice and evaluation of their cytotoxicity

L L Tsang et al. Cancer Chemother Pharmacol. 1990.

Abstract

The experimental antineoplastic agent temozolomide was not metabolised in vitro at a measurable rate by mouse liver fractions. In contrast, the temozolomide analogue 3-methylbenzotriazinone was metabolically N-demethylated by hepatic microsomes to yield benzotriazinone. The major route of excretion of [14C]-labelled temozolomide in mice was via the kidneys. An acidic metabolite of temozolomide, probably a conjugate, was found in the urine of mice, but its identity could not be established unambiguously. Spectroscopic analysis and chemical tests revealed that it possesses an intact NNN-linkage. Another metabolite was found in the urine of patients but not of mice. This metabolite was identified as the 8-carboxylic acid derivative of temozolomide. Unlike the unknown species, this metabolite was cytotoxic against TLX5 lymphoma cells in vitro.

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