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Comparative Study
. 1995;35(5):364-70.
doi: 10.1007/s002800050248.

D-19575--a sugar-linked isophosphoramide mustard derivative exploiting transmembrane glucose transport

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Comparative Study

D-19575--a sugar-linked isophosphoramide mustard derivative exploiting transmembrane glucose transport

J Pohl et al. Cancer Chemother Pharmacol. 1995.

Abstract

D-19575 is a glucose derivative of ifosfamide mustard with a broad spectrum of antitumor activity in animal models. In comparison with ifosfamide, D-19575 is less toxic and is better tolerated by tumor-bearing animals, achieving a better therapeutic efficacy. D-19575 is directly cytotoxic in vitro--in contrast to ifosfamide--and it is possible to modulate this cytotoxicity by inhibition of transmembrane glucose transporters. Correspondingly, renal reabsorption of filtered D-19575 could be blocked by pre- and cotreatment with phlorizin, resulting in a higher urinary excretion of the unchanged drug. The toxicity to white blood cells, colony-forming units (CFU-C), and spleen-cell colony-forming units (CFU-S) is considerably lower for D-19575 as compared with ifosfamide. In conclusion, D-19575 is a new alkylating cytotoxic agent with increased antitumor selectivity, probably caused by an active transmembrane transport mechanism.

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