• 作者：Xiaorong Sun^a ; ^b ; ¹ ; Ligang Xing^b ; ^c ; ¹ ; Xuelong Deng^b ; Hung Tsung Hsiao^b ; Akiko Manami^b ; Jason A. Koutcher^b ; C. Clifton Ling^b ; Gloria C. Li^b ; ^{lig@mskcc.org}
• 关键词：Hypoxia ; Radiosensitization ; Cytosine deaminase ; Uracil phosphoribosyltransferase ; 5-Flurocytosine
• 刊名：Radiotherapy and Oncology
• 出版年：2012
• 出版时间：October, 2012
• 年：2012
• 卷：105
• 期：1
• 页码：57-63
• 全文大小：1289 K

Purpose

Materials and methods

Stable transfectants of R3327-AT cells were established which express a triple-fusion-gene: CD, UPRT and monomoric DsRed (mDsRed) controlled by a hypoxia inducible promoter. Hypoxia-induced expression/function of CDUPRTmDsRed was verified by western blot, flow cytometry, fluorescent microscopy, and cytotoxicity assay of 5-FU and 5-FC. Tumor-bearing mice were treated with 5-FC and local radiation. Tumor volume was monitored and compared with those treated with 5-FC or radiation alone. In addition, the CDUPRTmDsRed distribution in hypoxic regions of tumor sections was visualized with fluorescent microscopy.

Results

Hypoxic induction of CDUPRTmDsRed protein correlated with increased sensitivity to 5-FC and 5-FU. Significant radiosensitization effects were detected after 5-FC treatments under hypoxic conditions. In the tumor xenografts, the distribution of CDUPRTmDsRed expression visualized with fluorescence microscopy was co-localized with the hypoxia marker pimonidazole positive staining cells. Furthermore, administration of 5-FC to mice in combination with local irradiation resulted in significant tumor regression, as in comparison with 5-FC or radiation treatments alone.

Conclusions

Our data suggest that the hypoxia-inducible CDUPRT/5-FC gene therapy strategy has the ability to specifically target hypoxic cancer cells and significantly improve the tumor control in combination with radiotherapy.