A 5‑FU Precursor Designed to Evade Anabolic and Catabolic Drug Pathways and Activated by Pd Chemistry In Vitro and In Vivo

5-Fluorouracil (5-FU) is an antineoplastic antimetabolite that is widely administered to cancer patients by bolus injection, especially to those suffering from colorectal and pancreatic cancer. Because of its suboptimal route of administration and dose-limiting toxicities, diverse 5-FU prodrugs have...

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Bibliographic Details
Published inJournal of medicinal chemistry Vol. 65; no. 1; pp. 552 - 561
Main Authors Adam, Catherine, Bray, Thomas L, Pérez-López, Ana M, Tan, Ee Hong, Rubio-Ruiz, Belén, Baillache, Daniel J, Houston, Douglas R, Salji, Mark J, Leung, Hing Y, Unciti-Broceta, Asier
Format Journal Article
LanguageEnglish
Published United States American Chemical Society 13.01.2022
Subjects
Animals
Antimetabolites, Antineoplastic - metabolism
Antimetabolites, Antineoplastic - toxicity
Biotransformation
Fluorouracil - analogs & derivatives
Fluorouracil - metabolism
Fluorouracil - toxicity
Half-Life
HCT116 Cells
Hepatocytes - drug effects
Hepatocytes - metabolism
Humans
Liver - metabolism
Metabolic Networks and Pathways - drug effects
Mice
Palladium - chemistry
Prodrugs - metabolism
Prodrugs - toxicity
Protein Binding
Rats
Xenograft Model Antitumor Assays
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Summary:5-Fluorouracil (5-FU) is an antineoplastic antimetabolite that is widely administered to cancer patients by bolus injection, especially to those suffering from colorectal and pancreatic cancer. Because of its suboptimal route of administration and dose-limiting toxicities, diverse 5-FU prodrugs have been developed to confer oral bioavailability and increase the safety profile of 5-FU chemotherapy regimens. Our contribution to this goal is presented herein with the development of a novel palladium-activated prodrug designed to evade the metabolic machinery responsible for 5-FU anabolic activation and catabolic processing. The new prodrug is completely innocuous to cells and highly resistant to metabolization by primary hepatocytes and liver S9 fractions (the main metabolic route for 5-FU degradation), whereas it is rapidly converted into 5-FU in the presence of a palladium (Pd) source. In vivo pharmokinetic analysis shows the prodrug is rapidly and completely absorbed after oral administration and exhibits a longer half-life than 5-FU. In vivo efficacy studies in a xenograft colon cancer model served to prove, for the first time, that orally administered prodrugs can be locally converted to active drugs by intratumorally inserted Pd implants.
ISSN:0022-2623
1520-4804
DOI:10.1021/acs.jmedchem.1c01733