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Nanoparticle delivery of a prodrug-activating bacterial enzyme leads to anti-tumor responses

Nature Communications. 2025-04; 
Sebastian G. Huayamares, Liming Lian, Regina Rab, Yuning Hou, Afsane Radmand, Hyejin Kim, Ryan Zenhausern, Bhagelu R. Achyut, Melissa Gilbert Ross, Melissa P. Lokugamage, David Loughrey, Hannah E. Peck, Elisa Schrader Echeverri, Alejandro J. Da Silva Sanchez, Aram Shajii, Andrea Li, Karen E. Tiegreen, Philip J. Santangelo, Eric J. Sorscher & James E. Dahlman Georgia Institute of Technology and Emory University School of Medicine
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Catalog Antibodies and MonoRabTM rabbit anti-camelid VHH antibody iFluor647 (A01994, GenScript), TotalSeq-A0259 (BioLegend 394617)]) and oligo-tagged anti-VHH antibody (5 µg/mL; A01860, GenScript). (CCTTGGCACCCGAGAATTCCAAAGTATGCCCTACGABAAAAAAAAAAAAAAAAAAAAAAAAAAAA*A*A, where * indicates phosphothioate bonds; GenScript) was conjugated to azide-modified rabbit anti-camelid VHH antibody (clone 96A3F5; GenScript) by click chemistry (GenScript). Get A Quote

Abstract

Most cancer patients diagnosed with late-stage head and neck squamous cell carcinoma are treated with chemoradiotherapy, which can lead to toxicity. One potential alternative is tumor-limited conversion of a prodrug into its cytotoxic form. We reason this could be achieved by transient and tumor-specific expression of purine nucleoside phosphorylase (PNP), an Escherichia coli enzyme that converts fludarabine into 2-fluoroadenine, a potent cytotoxic drug. To efficiently express bacterial PNP in tumors, we evaluate 44 chemically distinct lipid nanoparticles (LNPs) using species-agnostic DNA barcoding in tumor-bearing mice. Our lead LNP, designated LNP intratumoral (LNPIT), delivers mRNA that leads to PNP expressi... More

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