Facile route to targeted, biodegradable polymeric prodrugs for the delivery of combination therapy for Malaria

Fortuin, Lisa; Leshabane, Meta; Pfukwa, Rueben; Coertzen, Dina; Birkholtz, Lyn-Marie; Klumperman, Bert

Facile route to targeted, biodegradable polymeric prodrugs for the delivery of combination therapy for Malaria

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facile_fortuin_2020.pdf(3.27 MB)

Date

2020-06

Authors

Publisher

American Chemical Society

Abstract

A facile synthetic methodology has been developed to prepare multifaceted polymeric prodrugs that are targeted, biodegradable, and nontoxic, and used for the delivery of combination therapy. This is the first instance of the delivery of the WHO recommended antimalarial combination of lumefantrine (LUM, drug 1) and artemether (AM, drug 2) via a polymeric prodrug. To achieve this, reversible addition-fragmentation chain transfer (RAFT)-mediated polymerization of N-vinylpyrrolidone (NVP) was conducted using a hydroxy-functional RAFT agent, and the resulting polymer was used as the macroinitiator in the ring-opening polymerization (ROP) of α-allylvalerolactone (AVL) to synthesize the biodegradable block copolymer of poly(N-vinylpyrrolidone) and poly(α-allylvalerolactone) (PVP-b-PAVL). The ω-end thiol group of PVP was protected using 2,2′-pyridyldisulfide prior to the ROP, and was conveniently used to bioconjugate a peptidic targeting ligand. To attach LUM, the allyl groups of PVP-b-PAVL underwent oxidation to introduce carboxylic acid groups, which were then esterified with ethylene glycol vinyl ether. Finally, LUM was conjugated to the block copolymer via an acid-labile acetal linkage in a “click”-type reaction, and AM was entrapped within the hydrophobic core of the self-assembled aggregates to render biodegradable multidrug-loaded micelles with targeting ability for combination therapy.

Description

CITATION: Fortuin, L. et al. 2020. Facile route to targeted, biodegradable polymeric prodrugs for the delivery of combination therapy for Malaria. ACS Biomaterials Science & Engineering, 6(11): 6217-6227 doi:10.1021/acsbiomaterials.0c01234
The original publication is available at https://pubs.acs.org/journal/abseba

Keywords

Conjugated polymers, Polymeric drug delivery systems, Nanomedicine, Combined modality therapy, Malaria -- Prevention

Citation

Fortuin, L. et al. 2020. Facile route to targeted, biodegradable polymeric prodrugs for the delivery of combination therapy for Malaria. ACS Biomaterials Science & Engineering, 6(11): 6217-6227 doi:10.1021/acsbiomaterials.0c01234

URI

http://hdl.handle.net/10019.1/125226

Collections

Research Articles (Chemistry and Polymer Science)

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