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Simvastatin-nicotinamide co-crystal: design, preparation and preliminary characterization

机译:辛伐他汀-烟酰胺共晶体:设计,制备和初步表征

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Purpose: To improve the solubility of simvastatin (SV) by co-crystallization using nicotinamide (Nic) as co-crystal agent (co-former). Methods: In silico molecular modeling of Nic counter to SV were investigated using Auto Dock 4.2. Co-crystal of Nic-SV was obtained by solvent evaporation (SE) using an equimolar ratio of Nic and SV. Co-crystal of SV-Nic was evaluated by scanning electron microscopy (SEM), saturated solubility, intrinsic dissolution, x-ray powder diffraction (XRPD), differential scanning calorimetric (DSC), infrared spectrophotometry (FT-IR), binary phase diagram, and for stability at 40 oC and relative humidity (RH) 75% in one month. Results: In silico results showed that the interaction of Nic with SV took place through hydrogen bonding as the synthon agent. The solubility and intrinsic dissolution properties of the co-crystal improved significantly compared to pure SV. Characterization of the co-crystal SV: Nic (1: 1) by SEM, XRPD, DSC, FT-IR, and binary phase diagram indicate the formation of a new solid phase that was different from either SV or Nic. Furthermore, the cocrystal of SV: Nic remained stable for one month. Conclusion: Co-crystallization using Nic has the potential?to enhance drug solubility, intrinsic dissolution, and the stability of solution.
机译:目的:通过使用烟酰胺(Nic)作为共结晶剂(共形成剂)进行共结晶来提高辛伐他汀(SV)的溶解度。方法:使用Auto Dock 4.2研究了Nic对抗SV的计算机分子模型。使用Nic和SV的等摩尔比,通过溶剂蒸发(SE)获得Nic-SV的共晶体。通过扫描电子显微镜(SEM),饱和溶解度,本征溶解,X射线粉末衍射(XRPD),差示扫描量热法(DSC),红外分光光度法(FT-IR),二元相图评估SV-Nic的共晶,并在40摄氏度和相对湿度(RH)的15%内保持稳定。结果:计算机模拟结果表明,Nic与SV的相互作用是通过氢键作为合成子试剂进行的。与纯SV相比,该共晶体的溶解度和固有溶解特性显着提高。通过SEM,XRPD,DSC,FT-IR和二元相图表征SV:Nic(1:1)共晶,表明形成了不同于SV或Nic的新固相。此外,SV:Nic的共晶体保持稳定一个月。结论:使用Nic共结晶具有提高药物溶解度,固有溶解度和溶液稳定性的潜力。

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