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  • 2015년 10월호
    A Systematic Comparison of 18F-C-SNAT to Established Radiotracer Imaging Agents for the Detection of Tumor Response to Treatment.

    스탠포드대 / Timothy H. Witney, Sanjiv S. Gambhir*

  • 출처
    Clin Cancer Res.
  • 등재일
    2015 Sep 1
  • 저널이슈번호
    21(17):3896-905. doi: 10.1158/1078-0432.CCR-14-3176. Epub 2015 May 13.
  • 내용

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    PURPOSE:

    An early readout of tumor response to therapy through measurement of drug or radiation-induced cell death may provide important prognostic indications and improved patient management. It has been shown that the uptake of (18)F-C-SNAT can be used to detect early response to therapy in tumors by positron emission tomography (PET) via a mechanism of caspase-3-triggered nanoaggregation.

    EXPERIMENTAL DESIGN:

    Here, we compared the preclinical utility of (18)F-C-SNAT for the detection of drug-induced cell death to clinically evaluated radiotracers, (18)F-FDG, (99m)Tc-Annexin V, and (18)F-ML-10 in tumor cells in culture, and in tumor-bearing mice in vivo.

    RESULTS:

    In drug-treated lymphoma cells, (18)F-FDG, (99m)Tc-Annexin V, and (18)F-C-SNAT cell-associated radioactivity correlated well to levels of cell death (R(2) > 0.8; P < 0.001), with no correlation measured for (18)F-ML-10 (R(2) = 0.05; P > 0.05). A similar pattern of response was observed in two human NSCLC cell lines following carboplatin treatment. EL-4 tumor uptake of (99m)Tc-Annexin V and (18)F-C-SNAT were increased 1.4- and 2.1-fold, respectively, in drug-treated versus naïve control animals (P < 0.05), although (99m)Tc-Annexin V binding did not correlate to ex vivo TUNEL staining of tissue sections. A differential response was not observed with either (18)F-FDG or (18)F-ML-10.

    CONCLUSIONS:

    We have demonstrated here that (18)F-C-SNAT can sensitively detect drug-induced cell death in murine lymphoma and human NSCLC. Despite favorable image contrast obtained with (18)F-C-SNAT, the development of next-generation derivatives, using the same novel and promising uptake mechanism, but displaying improved biodistribution profiles, are warranted for maximum clinical utility.

     

    Author information

    Witney TH1, Hoehne A2, Reeves RE2, Ilovich O2, Namavari M2, Shen B2, Chin FT2, Rao J2, Gambhir SS2. 

    1Department of Radiology, Stanford University, Stanford, California. sgambhir@stanford.edu. 

    2Department of Radiology, Stanford University, Stanford, California.

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