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Metabolism and transport of oxazaphosphorines and the clinical implications

journal contribution
posted on 2024-11-01, 06:27 authored by J Zhang, Q Tian, SY Chan, Wei Duan, SC Li, YZ Zhu, Shufeng Zhou
The oxazaphosphorines including cyclophosphamide (CPA), ifosfamide (IFO), and trofosfamide represent an important group of therapeutic agents due to their substantial antitumor and immuno-modulating activity. CPA is widely used as an anticancer drug, an immunosuppressant, and for the mobilization of hematopoetic progenitor cells from the bone marrow into peripheral blood prior to bone marrow transplantation for aplastic anemia, leukemia, and other malignancies. New oxazaphosphorines derivatives have been developed in an attempt to improve selectivity and response with reduced toxicity. These derivatives include mafosfamide (NSC 345842), glufosfamide (D19575, beta-D-glucosylisophosphoramide mustard), NSC 612567 (aldophosphamide perhydrothiazine), and NSC 613060 (aldophosphamide thiazolidine). This review highlights the metabolism and transport of these oxazaphosphorines (mainly CPA and IFO, as these two oxazaphosphorine drugs are the most widely used alkylating agents) and the clinical implications. Both CPA and IFO are prodrugs that require activation by hepatic cytochrome P450 (CYP)-catalyzed 4-hydroxylation, yielding cytotoxic nitrogen mustards capable of reacting with DNA molecules to form crosslinks and lead to cell apoptosis and/or necrosis. Such prodrug activation can be enhanced within tumor cells by the CYP-based gene directed-enzyme prodrug therapy (GDEPT) approach

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Related Materials

  1. 1.
    DOI - Is published in 10.1080/03602530500364023
  2. 2.
    ISSN - Is published in 03602532

Journal

Drug Metabolism Reviews

Volume

37

Issue

4

Start page

611

End page

703

Total pages

93

Publisher

Informa Healthcare

Place published

United States

Language

English

Former Identifier

2006012998

Esploro creation date

2020-06-22

Fedora creation date

2010-12-06

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