| Literature DB >> 30952988 |
Walid S Kamoun1, Dmitri B Kirpotin1, Zhaohua Richard Huang1, Suresh K Tipparaju1, Charles O Noble1,2, Mark E Hayes1,2, Lia Luus1, Alexander Koshkaryev1, Jaeyeon Kim1, Ken Olivier1, Tad Kornaga1, Shinji Oyama1, Vasileios Askoxylakis1, Christine Pien1, Geoffrey Kuesters1, Nancy Dumont1, Alexey A Lugovskoy1, Sarah A Schihl3, John H Wilton3, Melissa L Geddie1, James Suchy1, Stephanie Grabow1, Neeraj Kohli1, C Patrick Reynolds4, Rachel Blaydes4, Yu Zhou5, Andrew J Sawyer1, James D Marks5, Daryl C Drummond6.
Abstract
Antibody-mediated tumour targeting and nanoparticle-mediated encapsulation can reduce the toxicity of antitumour drugs and improve their efficacy. Here, we describe the performance of a nanotherapeutic encapsulating a hydrolytically sensitive docetaxel prodrug and conjugated to an antibody specific for EphA2-a receptor overexpressed in many tumours. Administration of the nanotherapeutic in mice led to slow and sustained release of the prodrug, reduced exposure of active docetaxel in the circulation (compared with administration of the free drug) and maintenance of optimal exposure of the drug in tumour tissue. We also show that administration of the nanotherapeutic in rats and dogs resulted in minimal haematological toxicity, as well as the absence of neutropenia and improved overall tolerability in multiple rodent models. Targeting of the nanotherapeutic to EphA2 improved tumour penetration and resulted in markedly enhanced antitumour activity (compared with administration of free docetaxel and non-targeted nanotherapeutic controls) in multiple tumour-xenografted mice. This nanomedicine could become a potent and safe therapeutic alternative for cancer patients undergoing chemotherapy.Entities:
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Year: 2019 PMID: 30952988 DOI: 10.1038/s41551-019-0385-4
Source DB: PubMed Journal: Nat Biomed Eng ISSN: 2157-846X Impact factor: 25.671