Adaptation of targeted nanocarriers to changing requirements in antimalarial drug delivery.

Joana Marques; Juan José Valle-Delgado; Patricia Urbán; Elisabet Baró; Rafel Prohens; Alfredo Mayor; Pau Cisteró; Michael Delves ORCID logo; Robert E Sinden; Christian Grandfils; +3 more... José L de Paz; José A García-Salcedo; Xavier Fernàndez-Busquets; (2016) Adaptation of targeted nanocarriers to changing requirements in antimalarial drug delivery. Nanomedicine, 13 (2). pp. 515-525. ISSN 1549-9634 DOI: 10.1016/j.nano.2016.09.010
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The adaptation of existing antimalarial nanocarriers to new Plasmodium stages, drugs, targeting molecules, or encapsulating structures is a strategy that can provide new nanotechnology-based, cost-efficient therapies against malaria. We have explored the modification of different liposome prototypes that had been developed in our group for the targeted delivery of antimalarial drugs to Plasmodium-infected red blood cells (pRBCs). These new models include: (i) immunoliposome-mediated release of new lipid-based antimalarials; (ii) liposomes targeted to pRBCs with covalently linked heparin to reduce anticoagulation risks; (iii) adaptation of heparin to pRBC targeting of chitosan nanoparticles; (iv) use of heparin for the targeting of Plasmodium stages in the mosquito vector; and (v) use of the non-anticoagulant glycosaminoglycan chondroitin 4-sulfate as a heparin surrogate for pRBC targeting. The results presented indicate that the tuning of existing nanovessels to new malaria-related targets is a valid low-cost alternative to the de novo development of targeted nanosystems.


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