Liu Chengyu, Chen Zhen, Chen Yuejie, Lu Jia, Li Yuan, Wang Shujing, Wu Guoliang, Qian Feng
School of Pharmaceutical Sciences and Collaborative Innovation Center for Diagnosis and Treatment of Infectious Diseases, Tsinghua University , Beijing 100084, China.
College of Pharmaceutical Sciences, Soochow University , Suzhou 215006, China.
Mol Pharm. 2016 Feb 1;13(2):599-608. doi: 10.1021/acs.molpharmaceut.5b00837. Epub 2016 Jan 6.
Sorafenib is a clinically important oral tyrosine kinase inhibitor for the treatment of various cancers. However, the oral bioavailability of sorafenib tablet (Nexavar) is merely 38-49% relative to the oral solution, due to the low aqueous solubility of sorafenib and its relatively high daily dose. It is desirable to improve the oral bioavailability of sorafenib to expand the therapeutic window, reduce the drug resistance, and enhance patient compliance. In this study, we observed that the solubility of sorafenib could be increased ∼50-fold in the coexistence of poly(vinylpyrrolidone-vinyl acetate) (PVP-VA) and sodium lauryl sulfate (SLS), due to the formation of PVP-VA/SLS complexes at a lower critical aggregation concentration. The enhanced solubility provided a faster initial sorafenib dissolution rate, analogous to a forceful "spring" to release drug into solution, from tablets containing both PVP-VA and SLS. However, SLS appears to impair the ability of PVP-VA to act as an efficient "parachute" to keep the drug in solution and maintain drug supersaturation. Using 2D (1)H NMR, (13)C NMR, and FT-IR analysis, we concluded that the solubility enhancement and supersaturation of sorafenib were achieved by PVP-VA/SLS complexes and PVP-VA/sorafenib interaction, respectively, both through molecular interactions hinged on the PVP-VA VA groups. Therefore, a balance between "spring" and "parachute" must be carefully considered in formulation design. To confirm the in vivo relevance of these molecular interaction mechanisms, we prepared three tablet formulations containing PVP-VA alone, SLS alone, and PVP-VA/SLS in combination. The USP II in vitro dissolution and dog pharmacokinetic in vivo evaluation showed clear differentiation between these three formulations, and also good in vitro-in vivo correlation. The formulation containing PVP-VA alone demonstrated the best bioavailability with 1.85-fold and 1.79-fold increases in Cmax and AUC, respectively, compared with the formulation containing SLS only, the poorest performing one. Despite its forceful "spring", the formulation containing both PVP-VA and SLS showed a moderate bioavailability enhancement, due to the lack of an efficient "parachute".
索拉非尼是一种临床上重要的口服酪氨酸激酶抑制剂,用于治疗多种癌症。然而,由于索拉非尼的水溶性低且每日剂量相对较高,索拉非尼片剂(多吉美)的口服生物利用度相对于口服溶液仅为38%-49%。提高索拉非尼的口服生物利用度以扩大治疗窗口、降低耐药性并提高患者依从性是很有必要的。在本研究中,我们观察到在聚乙烯吡咯烷酮-醋酸乙烯酯(PVP-VA)和月桂醇硫酸酯钠(SLS)共存的情况下,索拉非尼的溶解度可提高约50倍,这是由于在较低的临界聚集浓度下形成了PVP-VA/SLS复合物。溶解度的提高使含有PVP-VA和SLS的片剂中索拉非尼的初始溶解速度更快,类似于一个有力的“弹簧”将药物释放到溶液中。然而,SLS似乎会损害PVP-VA作为有效“降落伞”将药物保持在溶液中并维持药物过饱和的能力。通过二维(1)H NMR、(13)C NMR和FT-IR分析,我们得出结论,索拉非尼溶解度的提高和过饱和分别是通过PVP-VA/SLS复合物和PVP-VA/索拉非尼相互作用实现的,两者均通过基于PVP-VA醋酸乙烯酯基团的分子相互作用。因此,在制剂设计中必须仔细考虑“弹簧”和“降落伞”之间的平衡。为了证实这些分子相互作用机制在体内的相关性,我们制备了三种片剂制剂,分别单独含有PVP-VA、单独含有SLS以及PVP-VA/SLS组合。美国药典II体外溶出度和犬体内药代动力学评价显示这三种制剂之间有明显差异,并且体外-体内相关性良好。单独含有PVP-VA的制剂表现出最佳的生物利用度,与表现最差的仅含有SLS 的制剂相比,其Cmax和AUC分别增加了1.85倍和1.79倍。尽管含有PVP-VA和SLS的制剂有有力的“弹簧”,但由于缺乏有效的“降落伞”,其生物利用度提高程度适中。
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