新型口服维拉帕米HCl基质片胃内性能及生物利用度研究。

Bollettino chimico farmaceutico Pub Date : 2003-09-01
Alaa Eldeen B Yassin, F Alkhaled, S al-Suwayeh, S Elkheshen
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摘要

在之前的研究中,我们开发了一种盐酸维拉帕米(VP)的口服缓释生物黏附基质片。该系统具有较强的生物粘附性和体外缓释特性。本研究的目的是评价制备的生物胶粘剂(B)的体内性能。beagle犬在给予含有12%硫酸钡的B后,腹部进行定期x射线成像,以评价胃内性能。对禁食的比格犬口服B后,在规定时间内采集的血液样本中VP的浓度进行了测定,并与给药商业VP缓释片(Manidon 120 R)后的血液样本进行了比较。x射线图像显示,生物胶粘剂在胃中几乎保持在相同的位置至少6小时,而对照片在1小时后消失。与Manidon相比,B的Cmax、tmax、AUC、t1/2和MRT之间无统计学差异。Manidon和B的Cmax分别为51.4 +/- 15.5和48.6 +/- 17.9 (ng/ml), tmax分别为7.0 +/- 1.9和6.0 +/- 0。AUCO -。Manidon和B分别为949.84 +/- 245.11和722.92 +/- 144.42 ng.h/ml。因此,制备的B片可以被认为是生物等效的商业曼尼冬迟缓产品。
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Intra-gastric performance and bioavailability study of a new per-oral bioadhesive Verapamil HCl matrix tablet in dogs.

In a previous study, we developed a per-oral extended--release bioadhesive matrix tablet for verapamil HCl (VP). The system combined both strong bioadhesion and sustained release properties in vitro. The purpose of this study is to evaluate the in vivo performance of the prepared bioadhesive tablets (B). The conduction of a periodic X-ray imaging of the abdomen of beagle dogs, after administration of B containing 12% barium sulfate, was used to evaluate the intra-gastric performance. The VP concentrations in blood samples taken at specified times after oral administration of B to fasted beagle dogs were determined and compared with those obtained after administration of a commercial sustained release VP tablets (Manidon 120 R). The X-ray images showed that bioadhesive tablets remained almost at the same place in the stomach for at least 6 hours while it disappeared after 1 hour in case of the control tablets. No statistical difference was seen between the Cmax, tmax, AUC, t1/2, and MRT for B compared to Manidon. The Cmax was found to be 51.4 +/- 15.5 and 48.6 +/- 17.9 (ng/ml) for Manidon and B, respectively and the corresponding tmax were 7.0 +/- 1.9 and 6.0 +/- 0, respectively. The AUCO-. for Manidon and B were 949.84 +/- 245.11 and 722.92 +/- 144.42 ng.h/ml, respectively. So, the prepared B tablets can be considered bioequivalent to the commercial Manidon Retard product.

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