Nanjing Tech University, Nanjing, Jiangsu Province, China.
AAPS PharmSciTech. 2019 Jan 2;20(1):37. doi: 10.1208/s12249-018-1216-8.
The purpose of this study was to research a novel combination of Plasdone-S630 and HPMCAS-HF as hot-melt carrier used in ziprasidone hydrochloride for enhanced oral bioavailability and dismissed food effect. Ziprasidone hydrochloride solid dispersion (ZH-SD) was prepared by hot-melt extrusion technique, and its optimized formulation was selected by the central composite design (CCD), which was characterized for powder X-ray diffraction (PXRD), fourier transform infrared spectroscopy (FTIR), in vitro dissolution study, and stability study. Finally, the in vivo study in fasted/fed state was carried out in beagle dogs. Based on PXRD analysis, HME technique successfully dispersed ziprasidone with a low crystallinity hydrochloride form in the polymers. According to the analysis of FTIR, hydrogen bonds were formed between drug and polymers during the process of HME. Without any noticeable bulk, crystalline could be found from the micrograph of ZH-SD when analyzed the result of scanning electron microscope (SEM). Pharmacokinetics studies indicated that the bioavailability of ZH-SD formulation had no significant difference in fasted and fed state, and the C and AUC of ZH-SD were two fold higher than Zeldox® in fasted state. This result indicated that ziprasidone has achieved a desired oral bioavailability in fasted state and no food effect.
本研究旨在研究 Plasdone-S630 和 HPMCAS-HF 的新型组合作为热熔载体用于盐酸齐拉西酮,以提高口服生物利用度并消除食物效应。采用热熔挤出技术制备盐酸齐拉西酮固体分散体(ZH-SD),并通过中心复合设计(CCD)选择其优化配方,通过粉末 X 射线衍射(PXRD)、傅里叶变换红外光谱(FTIR)、体外溶出度研究和稳定性研究对其进行表征。最后,在 Beagle 犬中进行了禁食/进食状态下的体内研究。基于 PXRD 分析,HME 技术成功地将低结晶度盐酸形式的齐拉西酮分散在聚合物中。根据 FTIR 分析,在 HME 过程中药物和聚合物之间形成了氢键。从扫描电子显微镜(SEM)的结果分析中可以发现,ZH-SD 的微观结构中没有明显的块状物,也没有发现晶体。药代动力学研究表明,ZH-SD 制剂在禁食和进食状态下的生物利用度无显著差异,且 C 和 AUC 在禁食状态下均是 Zeldox®的两倍。这一结果表明,齐拉西酮在禁食状态下达到了预期的口服生物利用度,且无食物效应。
