Adaptation of targeted nanocarriers to changing requirements in antimalarial drug delivery

被引：43

作者：

Marques, Joana ^{[1
,2
,3
,9
]}

Jose Valle-Delgado, Juan ^{[1
,2
,3
,10
]}

Urban, Patricia ^{[1
,2
,3
,11
]}

Baro, Elisabet ^{[1
,2
,3
]}

Prohens, Rafel ^{[4
]}

Mayor, Alfredo ^{[2
]}

Cistero, Pau ^{[2
]}

Delves, Michael ^{[5
]}

Sinden, Robert E. ^{[5
]}

Grandfils, Christian ^{[6
]}

de Paz, Jose L. ^{[7
]}

Garcia-Salcedo, Jose A. ^{[8
]}

Fernandez-Busquets, Xavier ^{[1
,2
,3
]}

机构：

[1] Inst Bioengn Catalonia IBEC, Nanomalaria Grp, Barcelona, Spain

[2] Univ Barcelona, Hosp Clin, Barcelona Ctr Int Hlth Res CRESIB, Barcelona Inst Global Hlth ISGlobal, Barcelona, Spain

[3] Univ Barcelona, Nanosci & Nanotechnol Inst IN2UB, Barcelona, Spain

[4] Univ Barcelona, Ctr Cient & Tecnol, Unitat Polimorfisme & Calorimetria, Barcelona, Spain

[5] Imperial Coll, Dept Life Sci, London, England

[6] Univ Liege, Interfacultary Res Ctr Biomat CEIB, Inst Chem, Liege, Sart Tilman, Belgium

[7] Ctr Invest Cient Isl La Cartuja, CSIC US, IIQ, Seville, Spain

[8] Univ Granada, Hosp Univ Granada, Inst Invest Biosanit Ibs Granada, Unidad Enfermedades Infecciosas & Microbiol, Granada, Spain

[9] IHMT, Rua Junqueira 100, P-1349008 Lisbon, Portugal

[10] Aalto Univ, Sch Chem Technol, Dept Forest Prod Technol, POB 16300, FI-00076 Aalto, Finland

[11] European Commiss, Joint Res Ctr, Inst Hlth & Consumer Protect, IT-21027 Ispra, VA, Italy

来源：

NANOMEDICINE-NANOTECHNOLOGY BIOLOGY AND MEDICINE | 2017年 / 13卷 / 02期

关键词：

Glycosaminoglycans; Malaria; Nanomedicine; Plasmodium; Targeted drug delivery; RED-BLOOD-CELLS; FALCIPARUM-INFECTED ERYTHROCYTES; PLASMODIUM-FALCIPARUM; CHONDROITIN-SULFATE; GLUCOSE-6-PHOSPHATE-DEHYDROGENASE DEFICIENCY; MALARIA TRANSMISSION; MEMBRANE PROTEIN-1; HEPARAN-SULFATE; IN-VITRO; ADHESION;

D O I：

10.1016/j.nano.2016.09.010

中图分类号：

TB3 [工程材料学];

学科分类号：

0805 ; 080502 ;

摘要：

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. (C) 2016 The Authors. Published by Elsevier Inc.

引用

页码：515 / 525

页数：11

共 60 条

[1] Inhibition of Plasmodium falciparum growth in vitro and adhesion to chondroitin-4-sulfate by the heparan sulfate mimetic PI-88 and other sulfated oligosaccharides [J].