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Spatial transcriptomic analysis drives PET imaging of tight junction protein expression in pancreatic cancer theranostics.

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Nature communications 📖 저널 OA 95.7% 2021: 2/2 OA 2022: 3/3 OA 2023: 3/3 OA 2024: 21/21 OA 2025: 202/202 OA 2026: 191/210 OA 2021~2026 2024 Vol.15(1) p. 10751
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Wang J, Seo JW, Kare AJ, Schneider M, Pandrala M, Tumbale SK

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Molecular imaging using positron emission tomography (PET) provides sensitive detection and mapping of molecular targets.

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APA Wang J, Seo JW, et al. (2024). Spatial transcriptomic analysis drives PET imaging of tight junction protein expression in pancreatic cancer theranostics.. Nature communications, 15(1), 10751. https://doi.org/10.1038/s41467-024-54761-6
MLA Wang J, et al.. "Spatial transcriptomic analysis drives PET imaging of tight junction protein expression in pancreatic cancer theranostics.." Nature communications, vol. 15, no. 1, 2024, pp. 10751.
PMID 39737976 ↗

Abstract

Molecular imaging using positron emission tomography (PET) provides sensitive detection and mapping of molecular targets. While cancer-associated fibroblasts and integrins have been proposed as targets for imaging of pancreatic ductal adenocarcinoma (PDAC), herein, spatial transcriptomics and proteomics of human surgical samples are applied to select PDAC targets. We find that selected cancer cell surface markers are spatially correlated and provide specific cancer localization, whereas the spatial correlation between cancer markers and immune-related or fibroblast markers is low. Claudin-4 expression increases ~16 fold in cancer as compared with normal pancreas, and tight junction localization confers low background for imaging in normal tissue. We develop a peptide-based molecular imaging agent targeted to claudin-4 with accumulation to ~25% injected activity per cubic centimeter (IA/cc) in metastases and ~18% IA/cc in tumors. Our work motivates a data-driven approach to selection of molecular targets.

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