Ultrasound-directed enzyme-prodrug therapy (UDEPT) using self-immolative doxorubicin derivatives
Roemhild, Karolin; Besse, Helena C.; Wang, Bi; Peña, Quim; Sun, Qingxue; Omata, Daiki; Ozbakir, Burcin; Bos, Clemens; Scheeren, Hans W.; Storm, Gert; Metselaar, Josbert M.; Yu, Haijun; Knüchel-Clarke, Ruth; Kiessling, Fabian; Moonen, Chrit T.W.; Deckers, Roel; Shi, Yang; Lammers, Twan
(2022) Theranostics, volume 12, issue 10, pp. 4791 - 4801
(Article)
Abstract
Background: Enzyme-activatable prodrugs are extensively employed in oncology and beyond. Because enzyme concentrations and their (sub)cellular compartmentalization are highly heterogeneous in different tumor types and patients, we propose ultrasound-directed enzyme-prodrug therapy (UDEPT) as a means to increase enzyme access and availability for prodrug activation locally. Methods: We synthesized β-glucuronidase-sensitive self-immolative
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doxorubicin prodrugs with different spacer lengths between the active drug moiety and the capping group. We evaluated drug conversion, uptake and cytotoxicity in the presence and absence of the activating enzyme β-glucuronidase. To trigger the cell release of β-glucuronidase, we used high-intensity focused ultrasound to aid in the conversion of the prodrugs into their active counterparts. Results: More efficient enzymatic activation was observed for self-immolative prodrugs with more than one aromatic unit in the spacer. In the absence of β-glucuronidase, the prodrugs showed significantly reduced cellular uptake and cytotoxicity compared to the parent drug. High-intensity focused ultrasound-induced mechanical destruction of cancer cells resulted in release of intact β-glucuronidase, which activated the prodrugs, restored their cytotoxicity and induced immunogenic cell death. Conclusion: These findings shed new light on prodrug design and activation, and they contribute to novel UDEPT-based mechanochemical combination therapies for the treatment of cancer.
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Keywords: Cancer, Focused ultrasound, HIFU, Prodrugs, β-glucuronidase, Glucuronidase/metabolism, Humans, Neoplasms/drug therapy, Prodrugs/pharmacology, Doxorubicin/therapeutic use, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Medicine (miscellaneous), Research Support, Non-U.S. Gov't, Journal Article
ISSN: 1838-7640
Publisher: Ivyspring International Publisher
Note: Funding Information: This work was supported by the European Research Council (ERC: Meta-Targeting (CoG 864121), PIcelles (PoC 813086), and Sound Pharma (Adv 268906)), the China Scholarship Council (CSC), the German Research Foundation (DFG: GRK 2375 (Tumor-targeted Drug Delivery; project number: 331065168), SFB 1066, LA2937/4-1 and SH 1223/1-1), and Era-NET EuroNanoMed-3 program (NSC4DIPG). Publisher Copyright: © The author(s). © The author(s).
(Peer reviewed)