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Prostate-Specific Membrane Antigen Targeted StarPEG Nanocarrier for Imaging and Therapy of Prostate Cancer.

Advanced healthcare materials/Advanced Healthcare Materials(2024)

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Abstract
The tumor uptake of large non-targeted nanocarriers primarily occurs through passive extravasation, known as the enhanced permeability and retention (EPR) effect. Prior studies demonstrated improved tumor uptake and retention of 4-arm 40 kDa star polyethylene glycol (StarPEG) polymers for cancer imaging by adding prostate-specific membrane antigen (PSMA) targeting small molecule ligands. To test PSMA-targeted delivery and therapeutic efficacy, StarPEG nanodrugs with/without three copies of PSMA-targeting ligands, ACUPA, are designed and synthesized. For single-photon emission computed tomography (SPECT) imaging and therapy, each nanocarrier is labeled with 177Lu using DOTA radiometal chelator. The radiolabeled nanodrugs, [177Lu]PEG-(DOTA)1 and [177Lu]PEG-(DOTA)1(ACUPA)3, are evaluated in vitro and in vivo using PSMA+ PC3-Pip and/or PSMA- PC3-Flu cell lines, subcutaneous xenografts and disseminated metastatic models. The nanocarriers are efficiently radiolabeled with 177Lu with molar activities 10.8-15.8 MBq/nmol. Besides excellent in vitro PSMA binding affinity (kD = 51.7 nM), the targeted nanocarrier, [177Lu]PEG-(DOTA)1(ACUPA)3, demonstrated excellent in vivo SPECT imaging contrast with 21.3% ID/g PC3-Pip tumors uptake at 192 h. Single doses of 18.5 MBq [177Lu]PEG-(DOTA)1(ACUPA)3 showed complete resolution of the PC3-Pip xenografts observed up to 138 days. Along with PSMA-targeted excellent imaging contrast, these results demonstrated high treatment efficacy of [177Lu]PEG-(DOTA)1(ACUPA)3 for prostate cancer, with potential for clinical translation. The multivalent StarPEG nanocarrier [177Lu]PEG-(DOTA)1(ACUPA)3 (ACUPA is ((S)-2-(3- ((S)-5-amino-1- carboxypentyl) ureido) pentanedioic acid) exhibits high prostate-specific membrane antigen (PSMA) targeted delivery of the therapeutic isotope 177Lu with superior imaging contrast and therapeutic efficacy in prostate cancer. In preclinical models, single-dose administration of the targeted nanocarrier shows a notable improvement in therapeutic efficacy compared to [177Lu]PSMA-617, suggesting potential for clinical translation in the future. image
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Key words
enhanced permeability and retention,polymer nanocarriers,prostate cancer,prostate-specific membrane antigen (PSMA),radioligand therapy,single photon excited computed tomography (SPECT) imaging
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