Design and Antifungal Activity of Fluconazole and Nystatin Loaded Onto Silica Mesoporous

被引:0
|
作者
Ali Arabi Monfared
Forough Karami
Ardeshir Shokrollahi
Somayeh Yazdanpanah
Taleb Sepehr
Kamiar Zomorodian
机构
[1] Shiraz University of Medical Sciences,Central Research Laboratory, SchoolofMedicine
[2] Yasouj University,Chemistry Department
[3] Shiraz University of Medical Sciences,Department of Medical Mycology and Parasitology, SchoolofMedicine
[4] Shiraz University of Medical Sciences,Student Research Committee, School of Medicine
[5] Basic Sciences in Infectious Diseases Research Center,School of Medicine
[6] Shiraz University of Medical Sciences,undefined
来源
Pharmaceutical Chemistry Journal | 2023年 / 57卷
关键词
antifungal activity; fluconazole; high-performance liquid chromatography; MCM-41; nystatin;
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中图分类号
学科分类号
摘要
The emerging resistance of fungal species and the limited number of available antifungals have resulted in many efforts to design novel agents for the management of fungal infections. In the current research, fluconazole (FLU) and nystatin (NYS) were loaded onto the mesoporous material of MCM-41-NH-pydc as a new drug delivery system in order to study their antifungal activities. Fourier transform infrared spectroscopy (FTIR), x-ray diffraction (XRD), and energy-dispersive x-ray spectrometry (EDX) analyses were applied to identify MCM-41-NH-pydc before and after immobilization of FLU and NYS. Moreover, the release of FLU and NYS from MCM-41-NH-pydc was measured by high-performance liquid chromatography (HPLC). The antifungal activity of NYS/FLU-loaded mesoporous material was determined against standard/azole-resistant Candida species using the broth microdilution method according to Clinical & Laboratory Standards Institute (CLSI) guidelines. The encapsulation efficiency for FLU@MCM-41-NH-pydc and NYS@MCM-41-NH-pydc were obtained as 1000 and 250_mg/g respectively. The XRD results indicated that the crystal phase of the mesoporous material was preserved after immobilization of FLU and NYS. The FTIR spectra of FLU@MCM-41-NH-pydc and NYS@MCM-41-NH-pydc revealed successful loading. Moreover, EDX analysis confirmed the structure of FLU@MCM-41-NH-pydc. According to the results, loading the FLU onto the mesoporous material has resulted in a significant increase in the geometric mean for minimum inhibitory concentration (GM MIC), whereas no statistically significant difference was found between the GM MIC values of NYS and NYS@MCM-41-NH-pydc. The release of both loaded antifungal drugs in a pH-dependent manner and the sustained release of NYS from the mesoporous material are considerable advantages of these newly designed formulations.
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页码:965 / 974
页数:9
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