Sodium Iodide Symporter (NIS)-Mediated Radiovirotherapy for Pancreatic Cancer

被引:62
作者
Penheiter, Alan R. [1 ]
Wegman, Troy R. [1 ]
Classic, Kelly L. [2 ]
Dingli, David [1 ,3 ]
Bender, Claire E. [4 ]
Russell, Stephen J. [1 ,3 ]
Carlson, Stephanie K. [1 ,4 ]
机构
[1] Mayo Clin, Dept Mol Med, Rochester, MN 55905 USA
[2] Mayo Clin, Sect Safety & Secur, Rochester, MN 55905 USA
[3] Mayo Clin, Div Hematol, Rochester, MN 55905 USA
[4] Mayo Clin, Dept Radiol, Rochester, MN 55905 USA
关键词
I-131; hNIS; measles virus; pancreatic cancer; sodium iodide symporter (NIS); HUMAN SODIUM/IODIDE SYMPORTER; CONCENTRATOR GENE-THERAPY; ENGINEERED MEASLES-VIRUS; THYROID-CANCER; CARCINOEMBRYONIC ANTIGEN; TARGETED RADIOTHERAPY; RADIOIODINE THERAPY; MULTIPLE-MYELOMA; PROSTATE-CANCER; VIRAL THERAPY;
D O I
10.2214/AJR.09.3672
中图分类号
R8 [特种医学]; R445 [影像诊断学];
学科分类号
1002 ; 100207 ; 1009 ;
摘要
OBJECTIVE. We have previously shown the therapeutic efficacy of an engineered oncolytic measles virus expressing the sodium iodide symporter reporter gene (MV-NIS) in mice with human pancreatic cancer xenografts. The goal of this study was to determine the synergy between MV-NIS-induced oncolysis and NIS-mediated I-131 radiotherapy in this tumor model. MATERIALS AND METHODS. Subcutaneous human BxPC-3 pancreatic tumors were injected twice with MV-NIS. Viral infection, NIS expression, and intratumoral iodide uptake were quantitated with I-123 micro-SPECT/CT. Mice with MV-NIS-infected tumors were treated with 0, 37, or 74 MBq I-131 and monitored for tumor progression and survival. Additional studies were performed with stable NIS-expressing tumors (BxPC-3-NIS) treated with 0, 3.7, 18.5, 37, or 74 MBq of I-131. RESULTS. Mice treated with intratumoral MV-NIS exhibited significant tumor growth delay (p < 0.01) and prolonged survival (p = 0.02) compared with untreated mice. Synergy between MV-NIS-induced oncolysis and NIS-mediated I-131 ablation was not seen; however, a significant correlation was observed between NIS-mediated intratumoral iodide localization (% ID/g) and peak tumor volume reduction (p = 0.04) with combination MV-NIS and I-131 therapy. Stably transduced NIS-expressing BxPC-3 tumors exhibited rapid regression with = 18.5 MBq I-131. CONCLUSION. Delivery of I-131 radiotherapy to NIS-expressing tumors can be optimized using micro-SPECT/CT imaging guidance. Significant hurdles exist for NIS as a therapeutic gene for combined radiovirotherapy in this human pancreatic cancer model. The lack of synergy observed with MV-NIS and I-131 in this model was not due to a lack of radiosensitivity but rather to a nonuniform intratumoral distribution of MV-NIS infection.
引用
收藏
页码:341 / 349
页数:9
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