维拉帕米对索非布韦兔肠原位吸收影响的研究。

Nada M Mohsen, Esmat E Zein El-Din, Mohamed A Osman, Shimaa M Ashmawy
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引用次数: 0

摘要

目的:索非布韦是一种核苷酸抗病毒药物,是生物制药分类系统(BCS) III类前药,由于其高亲水性和低肠通透性,肠道吸收有限。本研究旨在探讨索非布韦的腔内稳定性、解剖部位对其肠道吸收的影响以及维拉帕米对其吸收的影响。方法:采用家兔原位肠灌注技术,观察索非布韦在十二指肠、空肠、回肠和升结肠的吸收情况。这是在有维拉帕米和没有维拉帕米的情况下进行的。结果:肠内稳定性研究表明,索非布韦在不同肠段存在不同的降解组分。原位灌注数据显示索非布韦从小肠和大肠段吸收不完全。索非布韦单位长度吸收清除率(Pe.A . /L)记录值分别为0.026、0.0075、0.0026和0.054 ml/min。十二指肠、空肠、回肠和升结肠分别为Cm。Pe。A/L值大小顺序为结肠>十二指肠>空肠>回肠。这是P-gp在不同肠段含量的相反等级。索非布韦在十二指肠、空肠、回肠和升结肠完全吸收所需的长度分别为29.58、128.47、949.2和13.63 cm。维拉帕米共灌注可显著提高Pe。结论:除了多药丙型肝炎病毒(HCV)感染患者可能发生的药物相互作用外,索非布韦的吸收清除率与p -糖蛋白的含量相关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Investigation of the effect of verapamil on the regional absorption of sofosbuvir from rabbit intestine in situ.

Purpose: Sofosbuvir, a nucleotide antiviral drug, is a Biopharmaceutics Classification System (BCS) class III prodrug suffering from limited intestinal absorption due to its high hydrophilicity and low intestinal permeability. This research aims to investigate the luminal stability of Sofosbuvir, the influence of anatomical site on its intestinal absorption and the effects of verapamil on such absorption.

Method: The study utilized in situ rabbit intestinal perfusion technique to examine absorption of Sofosbuvir from duodenum, jejunum, ileum and ascending colon. This was conducted both with and without verapamil.

Results: The luminal stability study showed that Sofosbuvir was subjected to premature degradation with varying fractions degraded from the different intestinal segments. The in situ perfusion data showed incomplete absorption of Sofosbuvir from small and large intestinal segments. The recorded values of the absorptive clearance per unit length (Pe.A/L) of Sofosbuvir were 0.026, 0.0075, 0.0026, & 0.054 ml/min.cm for duodenum, jejunum, ileum, and ascending colon, respectively. The Pe.A/L values were ordered as colon > duodenum > jejunum > ileum. This is the opposite rank of P-gp content in the different intestinal segments. The recorded values of the length required for complete Sofosbuvir absorption (L95%) were 29.58, 128.47, 949.2 and, 13.63 cm for duodenum, jejunum, ileum, and ascending colon, respectively. Co-perfusion with verapamil significantly increased Pe.A/L and reduced the L95% of Sofosbuvir from both jejunum and ileum (P-value < 0.05).

Conclusion: The results indicated that the absorptive clearance of Sofosbuvir was site dependent and associated with the content of P-glycoprotein, in addition to the expected drug interactions that can occur in polymedicated hepatitis C virus (HCV) infected patients.

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