Open AccessJournal Article
Binding to Cellular Macromolecules as a Possible Mechanism for the Cytotoxicity of Misonidazole
A. J. Varghese,G. F. Whitmore +1 more
TLDR
In a number of tissues of C3H mice after administration of [14C]misonidazole, radioactivity was detected in the DNA, RNA, and protein fractions and it is postulated that nit mirroreduction and binding of the nitroreduction products to macromolecules is a probable mechanism for the mutagenic and cytotoxic properties of misonidrazole.Abstract:
Reduction of the nitro group occurred when [14C]misonidazole was treated with zinc dust in aqueous solution in the presence of ammonium chloride. When the reduction mixture was allowed to react with calf thymus DNA or bovine albumin, radioactivity was bound to both DNA and protein. Under the same conditions, misonidazole did not bind to these macromolecules. Analysis of the reduction mixture indicated that the hydroxylamine, amine, and hydrazo derivatives of mizonidazole were the major products. In a number of tissues of C3H mice after administration of [14C]misonidazole, radioactivity was detected in the DNA, RNA, and protein fractions. Similar results were also obtained with Chinese hamster ovary cells incubated with the drug in the absence of oxygen. It is postulated that nitroreduction and binding of the nitroreduction products to macromolecules is a probable mechanism for the mutagenic and cytotoxic properties of misonidazole.read more
Citations
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Imaging hypoxia to improve radiotherapy outcome
TL;DR: The potential use of imaging to help improve clinical outcome to radiotherapy is critically assessed to identify those patients on an individual basis who have hypoxic tumours and, thus, at the very least should receive some form of hypoxic modifier in conjunction with radiotherapy.
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Imaging of hypoxia in human tumors with [F-18]fluoromisonidazole.
Wui Jin Koh,Janet S. Rasey,Margaret L. Evans,John R. Grierson,Thomas K. Lewellen,Michael M. Graham,Kenneth A. Krohn,Thomas W. Griffin +7 more
TL;DR: The first experiences with PETT imaging of [F-18]FMISO uptake in human malignancies are presented, and the development of this technique as a tool for the non-invasive assessment of tumor hypoxia is described.
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Detection of Hypoxic Cells by Monoclonal Antibody Recognizing 2-Nitroimidazole Adducts
TL;DR: The use of this new compound and its highly specific monoclonal antibody may allow elucidation of bioreductive metabolism of the nitroheterocyclics and significantly improve technologies for the quantitation of tissue pO2.
Journal Article
Characteristics of the metabolism-induced binding of misonidazole to hypoxic mammalian cells.
J D Chapman,K Baer,J Lee +2 more
TL;DR: A large number of [14C]MISO adducts can be generated in hypoxic cells without any evidence of cytotoxicity, and they are slowly cleared from cells, which suggests that MISO preferentially binds to molecules within the cell in which it is metabolically activated.
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Characterization of radiolabeled fluoromisonidazole as a probe for hypoxic cells
Janet S. Rasey,Zdenka Grunbaum,Sara Magee,Norma J. Nelson,Peggy L. Olive,Ralph E. Durand,Kenneth A. Krohn +6 more
TL;DR: It is concluded that [18F]fluromisonidazole has potential use as a hypoxia imaging agent in vivo and binds stably in the same populations of hypoxic cells as does misonidrazole.
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Journal Article
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