Novel anthracycline-spacer-β-glucuronide, -β-glucoside, and -β-galactoside prodrugs for application in selective chemotherapy

A series of anthracycline prodrugs containing an immolative spacer was synthesized for application in selective chemotherapy. The prodrugs having the general structure anthracycline-spacer-beta-glycoside were designed to be activated by beta-glucuronidase or beta-galactosidase. Prodrugs with -chloro...

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Bibliographic Details
Published inBioorganic & medicinal chemistry Vol. 7; no. 8; pp. 1597 - 1610
Main Authors LEENDERS, R. G. G, DAMEN, E. W. P, BIJSTERVELD, E. J. A, SCHEEREN, H. W, HOUBA, P. H. J, VAN DER MEULEN-MUILEMAN, I. H, BOVEN, E, HAISMA, H. J
Format Journal Article
LanguageEnglish
Published Oxford Elsevier Science 01.08.1999
Subjects
Antibiotics, Antineoplastic - chemical synthesis
Antibiotics, Antineoplastic - chemistry
Antibiotics, Antineoplastic - pharmacokinetics
Antineoplastic agents
Biological and medical sciences
Biotransformation
Cell Division - drug effects
Drug Screening Assays, Antitumor
Galactosides - chemistry
General aspects
Glucosides - chemistry
Glucuronides - chemistry
Half-Life
Humans
Magnetic Resonance Spectroscopy
Medical sciences
Molecular Structure
Pharmacology. Drug treatments
Prodrugs - chemical synthesis
Prodrugs - chemistry
Prodrugs - pharmacokinetics
Tumor Cells, Cultured
Human
Antineoplastic agent
Nitro compound
Aldose
Benzene derivatives
Cytotoxicity
Prodrug
Organic carbamate
In vitro
Glucuroconjugate
Ovary
Position isomer
Cell line
Structure activity relation
Chlorine Organic compounds
Uronic acid
Anthracyclins
Bromine Organic compounds
Woman
Chemical synthesis
Tumor cell
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Summary:A series of anthracycline prodrugs containing an immolative spacer was synthesized for application in selective chemotherapy. The prodrugs having the general structure anthracycline-spacer-beta-glycoside were designed to be activated by beta-glucuronidase or beta-galactosidase. Prodrugs with -chloro, -bromo or -n-hexyl substituents on the spacer were synthesized as well as prodrugs containing a -beta-glucuronyl, -beta-glucosyl or -beta-galactosyl carbamate specifier. The key step in the synthesis of all prodrugs is the highly beta-diastereoselective addition reaction of the anomeric hydroxyl of a glycosyl donor to a spacer isocyanate resulting in the respective beta-glycosyl carbamate pro-moieties. The resulting protected pro-moieties were coupled to an anthracycline. Prodrugs were evaluated with respect to activation rate by the appropriate enzyme and additionally, their IC50 values were determined. Optimal prodrugs in this study were at least 100- to 200-fold less toxic than their corresponding drug in vitro and were activated to the parent drug in a half-life time of approximately 2 h.
ISSN:0968-0896
1464-3391
DOI:10.1016/S0968-0896(99)00095-4