溶解度
布洛芬
溶解
化学
差示扫描量热法
傅里叶变换红外光谱
核化学
粒径
扫描电子显微镜
粉末衍射
环糊精
色谱法
化学工程
材料科学
有机化学
结晶学
物理化学
药理学
医学
物理
复合材料
工程类
热力学
作者
Qurat-ul-ain Shoaib,Sumera Latif,Qazi Amir Ijaz,Hafsa Afzal,Muhammad Irfan Siddique,Amjad Hussain,Muhammad Sohail Arshad,Nadeem Irfan Bukhari,Nasir Abbas
出处
期刊:PubMed
日期:2021-05-01
卷期号:34 (3(Supplementary)): 1045-1055
被引量:4
摘要
In the present study nanotechnology approach, i.e., a cyclodextrin (CD) based carbonate nanosponge was used to improve the solubility and dissolution of ibuprofen. Solvent and ultrasound assisted methods were used to prepare nanosponges using two CDs (β-CD and 2-hydroxypropyl-β-CD (2HP-β-CD)) and a cross-linker (CL) diphenyl carbonate (DPC) in varying molar ratios. Nanosponges were investigated for their solubilizing efficiency and phase solubility studies. Structural analysis by Fourier transform infrared (FTIR) and powder X-ray diffraction (PXRD), thermo-analytical characterization by differential scanning calorimetry (DCS), morphology by scanning electron microscopy (SEM). In-vitro drug release followed by in-vivo analgesic and anti-inflammatory studies were performed. 2HP-β-CD based nanosponges (molar ratio 0.01:0.04) prepared by ultrasound assisted method showed the highest solubilizing efficiency (i.e., 4.28 folds). Stability constant values showed that all complexes were stable. Inclusion complexes of drug was confirmed by PXRD and DSC. SEM images showed porous structures confirming the formation of cross-linked network. Particle size was in the range of 296.8±64 to 611.7±32nm. In-vitro release studies showed enhanced dissolution profile from nanosponge formulation (~94% from I11) as compared to the pure drug (~45% Ibuprofen) in 120min. Significant (p<0.05) extent of pain inhibition and anti-inflammatory activity was observed for nanosponge formulation when compared with the pure drug. CD based carbonate nanosponges with better solubility, enhanced release profile, improved analgesic and anti-inflammatory activity were successfully formulated for ibuprofen.
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