Development and Evaluation of Peptide-Based [F]AlF-WT12 and [F]AlF-IPB-WT12 Radiotracers for Noninvasive PD-L1 Imaging in Tumor Models.
1/5 보강
PD-L1 in the immune checkpoint pathway is expressed on various tumor cells, and multiple PD-1/PD-L1 inhibitors have been approved for treating these malignancies.
APA
Mo C, Tan JE, et al. (2025). Development and Evaluation of Peptide-Based [F]AlF-WT12 and [F]AlF-IPB-WT12 Radiotracers for Noninvasive PD-L1 Imaging in Tumor Models.. Molecular pharmaceutics, 22(12), 7500-7512. https://doi.org/10.1021/acs.molpharmaceut.5c01032
MLA
Mo C, et al.. "Development and Evaluation of Peptide-Based [F]AlF-WT12 and [F]AlF-IPB-WT12 Radiotracers for Noninvasive PD-L1 Imaging in Tumor Models.." Molecular pharmaceutics, vol. 22, no. 12, 2025, pp. 7500-7512.
PMID
41222210 ↗
Abstract 한글 요약
PD-L1 in the immune checkpoint pathway is expressed on various tumor cells, and multiple PD-1/PD-L1 inhibitors have been approved for treating these malignancies. However, clinical studies indicate that only 20-30% of patients benefit from immunotherapy. To address this problem, two novel peptide-based radiotracers, [F]AlF-WT12 and [F]AlF-IPB-WT12, were developed within the present study. Both tracers were successfully prepared, with radiochemical yields of 15-25% and 25-35%, respectively ( > 5), and both exhibited high molar activities (17.97-30.11 GBq/μmol and 18.09-26.46 GBq/μmol, respectively). Their evaluation using in vivo PET imaging demonstrated significantly higher accumulation of both tracers in PD-L1-expressing 4T1-hPD-L1 and A549-hPD-L1 tumors compared to CHO control tumors. Notably, the [F]AlF-IPB-WT12 exhibited superior tumor uptake and prolonged retention time relative to [F]AlF-WT12. Additionally, good correlations were obtained between the PET imaging results and the results obtained from biodistribution studies and immunohistochemistry studies. Together, our findings demonstrate the promise of [F]AlF-IPB-WT12 as a tracer for noninvasive tumor imaging in clinical settings, with potential to guide immunotherapy decisions.
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