Investigation of the enhanced antitumour potency of STING agonist after conjugation to polymer nanoparticles

Investigation of the enhanced antitumour potency of STING agonist after conjugation to polymer nanoparticles

Intravenously administered cyclic dinucleotides and other STING agonists are hampered by low cellular uptake and poor circulatory half-life. Here we report the covalent conjugation of cyclic dinucleotides to poly(β-amino ester) nanoparticles through a cathepsin-sensitive linker. This is shown to inc...

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Veröffentlicht in:Nature nanotechnology 2023-11, Vol.18 (11), p.1351-1363
Hauptverfasser: Dosta, Pere, Cryer, Alexander M., Dion, Michelle Z., Shiraishi, Tsubasa, Langston, Steven P., Lok, David, Wang, Jianing, Harrison, Sean, Hatten, Tiquella, Ganno, Michelle L., Appleman, Vicky A., Taboada, Gonzalo Muñoz, Puigmal, Núria, Ferber, Shiran, Kalash, Santhosh, Prado, Michaela, Rodríguez, Alma L., Kamoun, Walid S., Abu-Yousif, Adnan O., Artzi, Natalie
Format: Artikel
Sprache:eng
Schlagworte:
140/131
631/61
631/61/54
Agonists
Animal models
Cancer
Chemistry and Materials Science
Conjugation
Immune clearance
Immune response
Immune system
Immunological memory
Immunotherapy
Materials Science
Melanoma
Nanoparticles
Nanotechnology
Nanotechnology and Microengineering
Polymers
Stability
Tumors
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