Synergistic antifungal activity against Candida albicans between voriconazole and cyclosporine a loaded in polymeric nanoparticles

被引:1
作者
Martin, Victoria [1 ]
de la Haba, Rafael R. [2 ]
Lopez-Cornejo, Pilar [1 ]
Lopez-Lopez, Manuel [3 ]
Lebron, Jose Antonio [1 ]
Bernal, Eva [1 ]
Baeza, Natalia [1 ]
Ruiz, Sara [1 ]
Ostos, Francisco Jose [1 ]
Merino-Bohorquez, Vicente [4 ]
Chevalier, Sylvie [5 ]
Lesouhaitier, Olivier [3 ]
Tahrioui, Ali [3 ]
Montes, Francisco Jose [1 ]
Sanchez-Carrasco, Teresa [1 ]
Moya, Maria Luisa [1 ]
机构
[1] Univ Seville, Dept Phys Chem, C Prof Garcia Gonzalez 1, Seville 41012, Spain
[2] Univ Seville, Fac Pharm, Dept Microbiol & Parasitol, C Prof Garcia Gonzalez 2, Seville 41012, Spain
[3] Univ Huelva, Fac Expt Sci, Dept Chem Engn Phys Chem & Mat Sci, Campus de El Carmen,Avda Fuerzas Armadas s-n, Huelva 21071, Spain
[4] Univ Seville, Dept Pharmacol, C-Prof Garcia Gonzalez 2, Seville 41012, Spain
[5] Univ Rouen Normandie, Normandie Univ, Univ Caen Normandie, CBSA UR4312, F-76000 Rouen, France
关键词
Cyclosporine A; PEG; PLGA; Polymeric nanoparticles; Synergism; Voriconazole; BIOFILM; FLUCONAZOLE; DELIVERY;
D O I
10.1016/j.ijpharm.2024.124593
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
The goal of this work is to investigate if the synergistic antifungal activity between cyclosporine A, CsA, and voriconazole, VRZ, increases when both drugs are encapsulated in a nanocarrier as compared when they are free. The preparation and characterization of blank and VRZ and CsA loaded polymeric based PLGA nanoparticles (PLGA, PLGA-PEG, and PLGA+PEG) was a necessary previous step. Using the more suitable NPs, those of PLGA, the antifungal susceptibility tests performed with VRZ-loaded PLGA NPs, show no significant increase of the antifungal activity in comparison to that of free VRZ. However, the synergistic behavior found for the (VRZ+CsA)-loaded PLGA NPs was fourfold stronger than that observed for the two free drugs together. On the other hand, the investigation into the suppression of C. albicans biofilm formation showed that blank PLGA NPs inhibit the biofilm formation at high NPs concentrations. However, a minor effect or even a slight biofilm increase formation was observed at low and moderate NPs concentrations. Therefore, the enhancement of the biofilm inhibition found for the three tested treatments (CsA alone, VRZ alone, and VRZ+CsA) when comparing free and encapsulated drugs, within the therapeutic window, can be attributed to the drug encapsulation approach. Indeed, polymeric PLGA NPs loaded with CsA, VRZ, or VRZ+CsA are more effective at inhibiting the C. albicans biofilm growth than their free counterparts.
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页数:10
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