American Association for Cancer Research
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Supplemental Figures S1-4 and Tables 1-2 from A Systematic Comparison of 18F-C-SNAT to Established Radiotracer Imaging Agents for the Detection of Tumor Response to Treatment

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journal contribution
posted on 2023-03-31, 18:31 authored by Timothy H. Witney, Aileen Hoehne, Robert E. Reeves, Ohad Ilovich, Mohammad Namavari, Bin Shen, Frederick T. Chin, Jianghong Rao, Sanjiv S. Gambhir

Supplemental Figures S1-4 and Tables 1-2. Supplemental Figure S1. Mechanism of 18F-C-SNAT activation, cyclization and intracellular trapping; Supplemental Figure S2. Flow cytometric analysis of cell death in EL-4 cell mixtures; Supplemental Figure S3. Radiotracer uptake and retention in carboplatin- and vehicle-treated PC9 and A549 non small cell lung cancer cells; Supplemental Figure S4. SPECT imaging of 99mTc-Annexin V uptake in vivo; Supplemental Table 1. Ex vivo biodistribution data for selected tissues in naive and drug-treated mice 90 min after injection; Supplemental Table 2. Radiotracer tumor-to-tissue ratios in naive and drug-treated EL-4 xenografts 90 min after injection.



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 18F-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 18F-C-SNAT for the detection of drug-induced cell death to clinically evaluated radiotracers, 18F-FDG, 99mTc-Annexin V, and 18F-ML-10 in tumor cells in culture, and in tumor-bearing mice in vivo.Results: In drug-treated lymphoma cells, 18F-FDG, 99mTc-Annexin V, and 18F-C-SNAT cell-associated radioactivity correlated well to levels of cell death (R2 > 0.8; P < 0.001), with no correlation measured for 18F-ML-10 (R2 = 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 99mTc-Annexin V and 18F-C-SNAT were increased 1.4- and 2.1-fold, respectively, in drug-treated versus naïve control animals (P < 0.05), although 99mTc-Annexin V binding did not correlate to ex vivo TUNEL staining of tissue sections. A differential response was not observed with either 18F-FDG or 18F-ML-10.Conclusions: We have demonstrated here that 18F-C-SNAT can sensitively detect drug-induced cell death in murine lymphoma and human NSCLC. Despite favorable image contrast obtained with 18F-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. Clin Cancer Res; 21(17); 3896–905. ©2015 AACR.