Literature DB >> 11215843

Fluorouracil and the new oral fluorinated pyrimidines.

J G Kuhn1.   

Abstract

OBJECTIVE: To briefly review the biotransformation and bioavailability of fluorouracil (5-FU); discuss the effects of dihydropyrimidine dehydrogenase (DpD) on the efficacy and toxicity profiles of 5-FU; and review a new class of drugs known collectively as the oral fluorinated pyrimidines, which inhibit or circumvent DpD activity and, when administered with 5-FU, alter its pharmacokinetic and pharmacodynamic properties. DATA SOURCES: A MEDLINE literature search was conducted (1966-March 1999) using the search terms fluoropyrimidines, fluorouracil, 5-FU, fluorinated pyrimidines, capecitabine, eniluracil, uracil-tegafur, uracil-ftorafur, UFT, S1, BMS-247616, and BOF-A2. Reference lists, bibliographies of pertinent articles, and abstracts from the American Society of Clinical Oncology and the San Antonio Breast Cancer Symposium annual meetings were also identified and reviewed. Both preclinical and clinical literature were reviewed and analyzed. DATA SYNTHESIS: The new oral fluorinated pyrimidines appear to produce antitumor activity equivalent or superior to that of intravenously administered 5-FU by achieving higher intratumoral 5-FU concentrations or sustained 5-FU exposure. These agents are generally associated with manageable and non-life-threatening toxicities. The oral route of administration facilitates ease of administration and may reduce total healthcare costs associated with 5-FU-sensitive tumors. More studies are needed to assess the therapeutic and economic benefits of the oral fluorinated pyrimidines.
CONCLUSIONS: The bioavailability, efficacy, and toxicity of 5-FU depend on its catabolic rate-limiting enzyme, The new oral fluorinated pyrimidines inhibit or circumvent DpD activity and, when combined with 5-FU, increase 5-FU's bioavailability and cytotoxic effects and decrease its toxicities. Results of Phase I and II studies in patients with a variety of malignancies suggest positive outcomes, including greater efficacy, less drug-related toxicity, lower costs related to drug administration, and greater patient convenience.

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Year:  2001        PMID: 11215843     DOI: 10.1345/aph.10096

Source DB:  PubMed          Journal:  Ann Pharmacother        ISSN: 1060-0280            Impact factor:   3.154


  10 in total

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2.  Implementing DPYD*2A Genotyping in Clinical Practice: The Quebec, Canada, Experience.

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Review 4.  Strategies for improving quality of life in older patients with metastatic breast cancer.

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5.  Role of caspases in 5-FU and selenium-induced growth inhibition of colorectal cancer cells.

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Review 6.  Evolving approaches to metastatic breast cancer patients pre-treated with anthracycline and taxane.

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7.  Bio- and Hemo-Compatible Silk Fibroin PEGylated Nanocarriers for 5-Fluorouracil Chemotherapy in Colorectal Cancer: In Vitro Studies.

Authors:  Ariana Hudiță; Ionuț Cristian Radu; Cătălin Zaharia; Andreea Cristina Ion; Octav Ginghină; Bianca Gălățeanu; Luminița Măruțescu; Florin Grama; Aristidis Tsatsakis; Leonid Gurevich; Marieta Costache
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8.  DTNQ-Pro, a Mimetic Dipeptide, Sensitizes Human Colon Cancer Cells to 5-Fluorouracil Treatment.

Authors:  Isabel Gomez-Monterrey; Pietro Campiglia; Ilaria Scognamiglio; Daniela Vanacore; Alessandra Dicitore; Angela Lombardi; Michele Caraglia; Ettore Novellino; Paola Stiuso
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9.  Higher expression of deoxyuridine triphosphatase (dUTPase) may predict the metastasis potential of colorectal cancer.

Authors:  A Kawahara; Y Akagi; S Hattori; T Mizobe; K Shirouzu; M Ono; T Yanagawa; M Kuwano; M Kage
Journal:  J Clin Pathol       Date:  2008-12-03       Impact factor: 3.411

10.  The effects of genomic polymorphisms in one-carbon metabolism pathways on survival of gastric cancer patients received fluorouracil-based adjuvant therapy.

Authors:  Tingting Zhao; Zhi Xu; Dongying Gu; Peng Wu; Xinying Huo; Xiaowei Wei; Yongfei Tang; Weida Gong; Ming-Liang He; Jinfei Chen
Journal:  Sci Rep       Date:  2016-07-26       Impact factor: 4.379

  10 in total

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