Comparison of Pharmacokinetic Characteristics of Bilosomal Dispersion Versus Pure Solution of Oral Ropinirole Hydrochloride in Rats

S. K. Ali, Entidhar J. Al-Akkam
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Abstract

Background: Ropinirole hydrochloride is a non-ergoline antiparkinson drug. It is a highly hydrophilic drug and classified as class III according to Biopharmaceutical Classification System with low absolute oral bioavailability of approximately 50% upon oral administration due to significant hepatic first-pass metabolism. Objective: to compare the pharmacokinetic parameters of Ropinirole,  when administered orally in the form of a Ropinirole bilosomal dispersion in contrast to an oral Ropinirole solution. Methods: This study involved the use of twelve male Wistar rats, with an average weight of 220±11 g, and these rats were divided into two groups, comprising six rats each. A 1.1mg/kg doses of pure Ropinirole and Ropinirole bilosomes were administered orally through gavage after reconstituting in distilled water. Ropinirole was quantified in the rat's plasma using HPLC, subsequently establishing a spiked calibration curve with plasma samples and utilizing paracetamol as an internal standard. The statistics included mean values (± SD; n = 6) for pharmacokinetic parameters, with statistical significance assessed using a Student's t-test. Results: For the oral bilosomes, the values were 9.4±0.11 μg /ml for Cmax, 3±0.00 h for Tmax, and 55.56±2.12 μg h/ml for AUC0-24. In contrast, for the oral solution, the corresponding values were 7.2±0.14 μg/ml for Cmax, 1.5±0.00 h for Tmax, and  23.70±2.23 μg h/ml for AUC0-24. These parameters were significantly higher (P<0.05) as compared with a pure drug solution. The comparative bioavailability of Ropinirole (AUC0-24 oral solution / AUC0-24 oral bilosomes ) is equal to 42.66%, which indicates the bioavailability of the oral RH solution was less than that of RH bilosomal dispersion. Conclusions: The use of nano vesicular carriers (bilosomes) shows significant potential as an effective delivery system for improving the oral bioavailability of ropinirole hydrochloride
大鼠口服盐酸罗匹尼罗双体分散液与纯溶液的药代动力学特性比较
背景:盐酸罗匹尼罗是一种非麦角碱类抗帕金森药物。目的:比较盐酸罗匹尼罗双体分散片与罗匹尼罗口服溶液的药代动力学参数:本研究使用 12 只雄性 Wistar 大鼠(平均体重 220±11 克),将这些大鼠分为两组,每组 6 只。将 1.1mg/kg 剂量的纯罗匹尼罗和罗匹尼罗双糖体在蒸馏水中重构后通过灌胃口服给药。采用高效液相色谱法对大鼠血浆中的罗匹尼罗进行定量,随后用血浆样本建立加标校准曲线,并使用扑热息痛作为内标。统计包括药代动力学参数的平均值(± SD;n = 6),统计显著性采用学生 t 检验:双管口服液的 Cmax 为 9.4±0.11 μg /ml,Tmax 为 3±0.00 h,AUC0-24 为 55.56±2.12 μg h/ml。相比之下,口服溶液的 Cmax 为 7.2±0.14 μg/ml,Tmax 为 1.5±0.00 h,AUC0-24 为 23.70±2.23 μg h/ml。与纯药物溶液相比,这些参数明显更高(P<0.05)。罗匹尼罗的比较生物利用度(AUC0-24 口服溶液/AUC0-24 口服双糖体)等于 42.66%,这表明 RH 口服溶液的生物利用度低于 RH 双糖体分散液:纳米囊状载体(双体)作为一种有效的给药系统,在提高盐酸罗匹尼罗的口服生物利用度方面具有巨大潜力。
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