洛匹那韦-薄荷醇共晶体用于提高溶解速率和肠道吸收。
Lopinavir-menthol co-crystals for enhanced dissolution rate and intestinal absorption.
作者信息
Fayed Noha D, Arafa Mona F, Essa Ebtesam A, El Maghraby Gamal M
机构信息
Department of Pharmaceutical Technology, Faculty of Pharmacy, University of Tanta, Tanta, Egypt.
出版信息
J Drug Deliv Sci Technol. 2022 Aug;74:103587. doi: 10.1016/j.jddst.2022.103587. Epub 2022 Jul 11.
Lopinavir is an antiretroviral, antiparasitic agent and recently utilized in treatment of COVID-19. Unfortunately, lopinavir exhibited poor oral bioavailability due to poor dissolution, extensive pre-systemic metabolism, and significant P-glycoprotein intestinal efflux. Accordingly, the aim was to enhance dissolution rate and intestinal absorption of lopinavir. This employed co-processing with menthol which is believed to modify crystalline structures and inhibit intestinal efflux. Lopinavir was mixed with menthol at different molar ratios before ethanol assisted kneading. Formulations were evaluated using FTIR spectroscopy, differential scanning calorimetry (DSC), X-ray powder diffraction (XRD) and dissolution studies. Optimum ratio was utilized to assess lopinavir intestinal permeability. This employed in situ rabbit intestinal perfusion technique. FTIR, DSC and XRD indicated formation of lopinavir-menthol co-crystals at optimum molar ratio of 1:2. Additional menthol underwent phase separation due to possible self-association. Co-crystallization significantly enhanced lopinavir dissolution rate compared with pure drug to increase the dissolution efficiency from 24.96% in case of unprocessed lopinavir to 91.43% in optimum formulation. Lopinavir showed incomplete absorption from duodenum and jejuno-iliac segments with lower absorptive clearance from jejuno-ileum reflecting P-gp efflux. Co-perfusion with menthol increased lopinavir intestinal permeability. The study introduced menthol as co-crystal co-former for enhanced dissolution and augmented intestinal absorption of lopinavir.
洛匹那韦是一种抗逆转录病毒、抗寄生虫药物,最近被用于治疗新冠肺炎。不幸的是,由于溶解性差、广泛的首过代谢以及显著的P-糖蛋白肠道外排,洛匹那韦的口服生物利用度较差。因此,目的是提高洛匹那韦的溶解速率和肠道吸收。这采用了与薄荷醇共同加工的方法,据信薄荷醇可改变晶体结构并抑制肠道外排。在乙醇辅助捏合之前,将洛匹那韦与薄荷醇以不同的摩尔比混合。使用傅里叶变换红外光谱(FTIR)、差示扫描量热法(DSC)、X射线粉末衍射(XRD)和溶出度研究对制剂进行评估。利用最佳比例评估洛匹那韦的肠道通透性。这采用了原位兔肠道灌注技术。FTIR、DSC和XRD表明,在1:2的最佳摩尔比下形成了洛匹那韦-薄荷醇共晶体。由于可能的自缔合,额外的薄荷醇发生了相分离。与纯药物相比,共结晶显著提高了洛匹那韦的溶解速率,使溶解效率从未加工洛匹那韦的24.96%提高到最佳制剂的91.43%。洛匹那韦在十二指肠和空肠-回肠段的吸收不完全,空肠-回肠的吸收清除率较低,反映了P-糖蛋白外排。与薄荷醇共同灌注可提高洛匹那韦的肠道通透性。该研究引入薄荷醇作为共晶共形成剂,以提高洛匹那韦的溶解和增强肠道吸收。
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