Nanoparticulated Systems Based on Natural Polymers Loaded with Miconazole Nitrate and Lidocaine for the Treatment of Topical Candidiasis

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作者
G. Tejada
M. G. Barrera
P. García
M. Sortino
M. C. Lamas
V. Lassalle
V. Alvarez
D. Leonardi
机构
[1] IQUIR-CONICET,Área Técnica Farmacéutica, Departamento Farmacia, Facultad de Ciencias Bioquímicas y Farmacéuticas
[2] Universidad Nacional de Rosario,Planta Piloto de Producción de Medicamentos, Facultad de Ciencias Bioquímicas y Farmacéuticas
[3] Universidad Nacional de Rosario,Centro de Referencia de Micología (CEREMIC), Área Farmacognosia, Departamento Química Orgánica, Facultad de Ciencias Bioquímicas y Farmacéuticas
[4] Universidad Nacional de Rosario,Departamento de Química
[5] Instituto de Química del Sur (INQUISUR-UNS-CONICET),Facultad de Ingeniería
[6] Universidad Nacional del Sur,undefined
[7] Grupo Materiales Compuestos Termoplásticos (CoMP) Instituto de Investigaciones en Ciencia y Tecnología de Materiales (INTEMA),undefined
[8] Universidad Nacional de Mar Del Plata (UNMdP) y Consejo Nacional de Ciencia y Tecnología de Materiales (CONICET),undefined
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关键词
chitosan; gelatin; nano-particle; antifungal;
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摘要
People with weakened immune systems are at risk of developing candidiasis which is a fungal infection caused by several species of Candida genus. In this work, polymeric nanoparticles containing miconazole nitrate and the anesthetic lidocaine clorhydrate were developed. Miconazole was chosen as a typical drug to treat buccopharyngeal candidiasis whereas lidocaine may be useful in the management of the pain burning, and pruritus caused by the infection. Nanoparticles were synthesized using chitosan and gelatin at different ratios ranging from 10:90 to 90:10. The nano-systems presented nanometric size (between 80 and 300 nm in water; with polydispersion index ranging from 0.120 to 0.596), and positive Z potential (between 20.11 and 37.12 mV). The determined encapsulation efficiency ranges from 65 to 99% or 34 to 91% for miconazole nitrate and lidocaine clorhydrate, respectively. X-ray diffraction and DSC analysis suggested that both drugs were in amorphous state in the nanoparticles. Finally, the systems fitted best the Korsmeyer–Peppas model showing that the release from the nanoparticles was through diffusion allowing a sustained release of both drugs and prolonged the activity of miconazole nitrate over time against Candida albicans for at least 24 h.
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