Lipophilic Prodrugs and Formulations of Conventional (Deoxy)Nucleoside and Fluoropyrimidine Analogs in Cancer |
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Authors: | Godefridus J. Peters Auke D. Adema Irene V. Bijnsdorp Marit L. Sandvold |
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Affiliation: | 1. Department of Medical Oncology , VU University Medical Center , Amsterdam, The Netherlands;2. Department of Medical Oncology , VU University Medical Center , Amsterdam, The Netherlands;3. Department of Urology , VU University Medical Center , Amsterdam, The Netherlands;4. Clavis Pharma , Oslo, Norway |
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Abstract: | Many drugs that are currently used for the treatment of cancer have limitations, such as induction of resistance and/or poor biological half-life, which reduce their clinical efficacy. To overcome these limitations, several strategies have been explored. Chemical modification by the attachment of lipophilic moieties to (deoxy)nucleoside analogs should enhance the plasma half-life, change the biodistribution, and improve cellular uptake of the drug. Attachment of a lipophilic moiety to a phosphorylated (deoxy)nucleoside analog will improve the activity of the drugs by circumventing the rate-limiting activation step of (deoxy)nucleoside analogs. Encapsulating drugs in nanoparticles or liposomes protects the drug against enzymatic breakdown in the plasma and makes it possible to get lipophilic compounds to the tumor site. In this review, we discuss the considerable progress that has been made in increasing the efficacy of classic (deoxy)nucleoside and fluoropyrimidine compounds by chemical modifications and alternative delivery systems. |
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Keywords: | Deoxynucleoside analogs fluoropyrimidine analogs drug targeting nanoparticles liposomes lipophilic prodrugs |
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