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首页> 外文期刊>RSC Advances >Improving the solubility and bioavailability of anti-hepatitis B drug PEC via PEC–fumaric acid cocrystal
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Improving the solubility and bioavailability of anti-hepatitis B drug PEC via PEC–fumaric acid cocrystal

机译:通过PEC-富马酸COCrystal改善抗乙型肝炎药物PEC的溶解度和生物利用度

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摘要

PEC is a new generation of phosphamide ester anti-hepatitis B virus drug. It is a prodrug of tenofovir and can be rapidly metabolized to tenofovir. However, its poor solubility in water (0.219 mg mL ~(?1) at 25 °C) has limited its oral bioavailability. In this study, we aimed to improve the solubility and consequently the oral bioavailability of PEC via a cocrystal. A cocrystal of PEC with fumaric acid (FUA) (PEC–FUA, 1?:?1) was successfully obtained and characterized. The crystal structure of this cocrystal was tested using a single crystal X-ray diffraction method. The intrinsic dissolution rate (IDR) characterization was performed in a pH 6.8 buffer. The solubility of this cocrystal in 0.1 M HCl (pH 1.0) and pH 6.8 phosphate buffers was investigated, and the results showed that the solubility of the cocrystal was 3.8 and 4.0 times that of free PEC, respectively. We also studied the pharmacokinetics of beagle dogs. The mean AUC _(0–24 h) of the cocrystal is about 4.2 times that of free PEC, indicating that the solubility and bioavailability of PEC can indeed be improved by forming the cocrystal. It may become an ideal solid form of an active pharmaceutical ingredient suitable for pharmaceutical preparations, and it can be further studied later.
机译:PEC是一代新一代磷酸磷酸酯抗乙型肝炎病毒药物。它是替诺福韦的前药,可以迅速代谢到替诺福韦。然而,它在水中的溶解度不佳(25℃下0.219mg ml〜(α1))限制其口服生物利用度。在这项研究中,我们旨在改善溶解度,从而通过COCrystal来改善PEC的口服生物利用度。成功地获得了具有富马酸(FUA)(PEC-FUA,1?:1)的PEC的COCrystal。使用单晶X射线衍射法测试该聚碳晶的晶体结构。在pH 6.8缓冲液中进行内在溶解速率(IDR)表征。研究了该聚碳基在0.1M HCl(pH 1.0)和pH6.8磷酸盐缓冲液中的溶解度,结果表明,COCrystal的溶解度分别为3.8%和4.0倍的游离PEC。我们还研究了比格犬的药代动力学。 COCRYSTAL的平均AUC _(0-24h)是游离PEC的约4.2倍,表明通过形成COCRYSTAL,可以确实改善PEC的溶解度和生物利用度。它可能成为适用于药物制剂的活性药物成分的理想实心形式,并且可以在后面进一步研究。

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