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  • engineering of a nanostructured lipid carrier for the poorly water-soluble drug, bicalutamide: physicochemical investigations

    جزئیات بیشتر مقاله
    • تاریخ ارائه: 1392/07/24
    • تاریخ انتشار در تی پی بین: 1392/07/24
    • تعداد بازدید: 983
    • تعداد پرسش و پاسخ ها: 0
    • شماره تماس دبیرخانه رویداد: -
     the purpose of this study was to develop an optimized nanostructured lipid carrier (nlc) for bicalutamide (bct), a poorly water-soluble drug, and to investigate its phase transition behavior during the nlc processing. bct loaded nlcs (bct-nlcs) were prepared using a hot high-pressure homogenization (hph) technique. factorial design (23) was used to identify the key formulation variables influencing particle size, percent drug encapsulation, and zeta potential of the nlc. the optimized batch (nlc-2) revealed spherical morphology with a smooth surface under scanning electron microscopy (sem). nlc-2 achieved a high drug encapsulation of 98.48 ± 0.70% and demonstrated good stability for six months. drug–lipid interaction was investigated using fourier transform infrared spectra (ft-ir) and proton nuclear magnetic resonance (1h nmr). bct phase transition occurred during the nlc processing and bct crystalline form i was identified in nlc-2. the same was confirmed by differential scanning calorimetry (dsc), powder x-ray diffraction (pxrd), and raman analysis. the in vitro release study of nlc-2, revealed peppas release kinetics with fickian diffusion (n < 0.5) as drug release mechanism. the presence of hydrophilic surfactants was significant to modulate bct release from nlc-2. finally, nlcs made of precirol® ato 5 (solid lipid) and triacetin (oil) posses the potential to entrap the poorly water-soluble drug, bicalutamide and the system can be tailor-made to meet the desired drug release. this may provide better prospects for the oral delivery of bicalutamide.

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