Evaluation of tempol radioprotection in a murine tumor model

Stephen M. Hahn, Francis J. Sullivan, Anne Marie DeLuca, C. Murali Krishna, Nancy Wersto, David Venzon, Angelo Russo, James B. Mitchell

Research output: Contribution to a Journal (Peer & Non Peer)Articlepeer-review

84 Citations (Scopus)

Abstract

Tempol, a stable nitroxide free radical compound, is an in vitro and in vivo radioprotector. Previous studies have shown that Tempol protects C3H mice against whole-body radiation-induced bone marrow failure. In this study, the radioprotection of tumor tissue was evaluated. RIF-1 tumor cells were implanted in female C3H mice 10 d prior to radiation. Groups of mice were injected intraperitoneally with Tempol (275 mg/kg) or PBS followed 10 min later by a single dose of radiation to the tumor bed. Tumor growth curves generated after 10 and 33.3 Gy doses of radiation showed no difference in growth between the Tempol- and PBS-treated animals. A full radiation dose- response experiment revealed a tumor control dose in 50% of the animals in 30 d (TCD(50/30)) value of 36.7 Gy for Tempol-treated mice and 41.8 Gy for saline-treated mice suggesting no protection of the RIF-1 tumor by Tempol. Tumor pharmacokinetics were done to determine why Tempol differentially protected bone marrow and not tumor cells. Differential reduction of Tempol in the RIF-1 tumor and bone marrow was evaluated with EPR spectroscopy 10, 20, and 30 min after injection. Bioreduction of Tempol to its corresponding hydroxylamine (which is not a radioprotector) occurred to a greater extent in RIF-1 tumor cells compared to bone marrow. We conclude that the differences in radioprotection may result from enhanced intratumor bioreduction of Tempol to its nonradioprotective hydroxylamine analogue. The nitroxides as a class of compounds may provide a means to exploit the redox differences between normal tissues and tumors.

Original languageEnglish
Pages (from-to)1211-1216
Number of pages6
JournalFree Radical Biology and Medicine
Volume22
Issue number7
DOIs
Publication statusPublished - 1997
Externally publishedYes

Keywords

  • Bioreduction
  • Free radicals
  • Nitroxides
  • Radioprotection
  • Tumor control
  • Tumor regrowth

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