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Intraoral Mitochondrial-Targeted GS-Nitroxide, JP4-039, Radioprotects Normal Tissue in Tumor-Bearing Radiosensitive Fancd2–/– (C57BL/6) Mice

Authors :
Peter Wipf
Hong Wang
Darcy Franicola
Donna Shields
Xiaolan Zhang
Julie P. Goff
Song Li
Hebist Berhane
Robert L. Ferris
Joel S. Greenberger
Ronny Kalash
Karen M. Xu
Valerian E. Kagan
Xichen Zhang
Michael W. Epperly
Kalindi Parmar
Tracy Dixon
Vladimir A. Tyurin
Eva C. Guinan
Ashwin Shinde
Byung Han Rhieu
Source :
Radiation Research. 185:134
Publication Year :
2016
Publisher :
Radiation Research Society, 2016.

Abstract

We evaluated normal tissue specific radioprotection of the oral cavity in radiosensitive Fanconi Anemia (FA) Fancd2(-/-) mice with orally established tumors using mitochondrial-targeted GS-nitroxide (JP4-039). Adult (10-12 weeks old) Fancd2(+/+), Fancd2(+/-) and Fancd2(-/-) mice (C57BL/6 background) and subgroups with orally established TC-1 epithelial cell tumors received a single fraction of 28 Gy or four daily fractions of 8 Gy to the head and neck. Subgroups received JP4-039 in F15 emulsion (F15/JP4-039; 0.4 mg/mouse), 4-amino-Tempo in F15 emulsion (F15/4-amino-Tempo; 0.2 mg/mouse) or F15 emulsion alone prior to each irradiation. Oral mucosa of Fancd2(-/-) mice showed baseline elevated RNA transcripts for Sod2, p53, p21 and Rad51 (all P0.0012) and suppressed levels of Nfkb and Tgfb, (all P0.0020) compared with Fancd2(+/+) mice. The oral mucosa in tumor-bearing mice of all genotypes showed decreased levels of p53 and elevated Tgfb and Gadd45a (P ≤ 0.0001 for all three genotypes). Intraoral F15/JP4-039, but not F15/4-amino-Tempo, modulated radiation-induced normal tissue transcript elevation, ameliorated mucosal ulceration and reduced the depletion of antioxidant stores in oral cavity tissue of all genotypes, but did not radioprotect tumors. Mitochondrial targeting makes F15/JP4-039 an effective normal tissue radioprotector for Fancd2(-/-) mice, as well as wild-type mice.

Details

ISSN :
00337587
Volume :
185
Database :
OpenAIRE
Journal :
Radiation Research
Accession number :
edsair.doi.dedup.....d8ff2000a8f2660714074ae8f77521be
Full Text :
https://doi.org/10.1667/rr14035.1