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阿立哌唑的溶液介导的相转变:否定晶型对溶解和口服药代动力学的影响。

Solution-Mediated Phase Transformation of Aripiprazole: Negating the Effect of Crystalline Forms on Dissolution and Oral Pharmacokinetics.

机构信息

College of Pharmacy, CHA University, Seongnam 13844, Korea.

College of Pharmacy, CHA University, Seongnam 13844, Korea.

出版信息

J Pharm Sci. 2020 Dec;109(12):3668-3677. doi: 10.1016/j.xphs.2020.09.031. Epub 2020 Sep 29.

Abstract

We aimed to evaluate the effect of crystalline forms of aripiprazole, an antipsychotic drug for schizophrenia, on the dissolution rates and oral pharmacokinetics. Solubility, intrinsic dissolution rates, and tablet dissolution rates of the monohydrate (MA) and the anhydrous form (AA) were measured in various aqueous media while monitoring the phase transformation by ATR-FTIR. And their oral pharmacokinetics in dogs were compared. The intrinsic dissolution rate of MA was lower compared to AA, confirming its thermodynamic stability relative to AA in water. Phase transformations during the solubility measurement were media-dependent: In simulated gastric fluid, both AA and MA changed to HCl salt form, whereas AA and HCl salt form transformed to MA in simulated intestinal fluid. In vitro dissolution rates and dog oral pharmacokinetics of AA and MA tablets were similar. The results suggest that the solution-mediated transformation to HCl salt or MA negates the effect of different crystalline forms on dissolution rates in vivo and, consequently, on oral pharmacokinetics. We emphasize the importance of the dissolution tests employing various bio-relevant media for better prediction of in vivo performance and the selection of a solid form for development.

摘要

我们旨在评估抗精神分裂症药物阿立哌唑的晶型对其溶解速率和口服药代动力学的影响。在监测ATR-FTIR 下的相转变的同时,在各种水介质中测量一水合物 (MA) 和无水形式 (AA) 的溶解度、内在溶解速率和片剂溶解速率。并比较它们在狗体内的口服药代动力学。与 AA 相比,MA 的内在溶解速率较低,这证实了其在水中相对于 AA 的热力学稳定性。在溶解度测量过程中的相转变是依赖于介质的:在模拟胃液中,AA 和 MA 都转变为 HCl 盐形式,而在模拟肠液中,AA 和 HCl 盐形式转变为 MA。AA 和 MA 片剂的体外溶解速率和狗的口服药代动力学相似。结果表明,溶液介导的向 HCl 盐或 MA 的转化否定了不同晶型对体内溶解速率以及口服药代动力学的影响。我们强调了使用各种生物相关介质进行溶解试验的重要性,以便更好地预测体内性能并选择用于开发的固体形式。

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