包合物作为提高奥美沙坦-美多索米口服生物利用度的潜在体系的研究

Hetal Thakkar, B. V. Patel, M. Parmar, Nirav P Chauhan, Arpita A Patel
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引用次数: 10

摘要

背景:口服降压药奥美沙坦美多索米(OLM)由于水溶性较差(7.75 μg/ml),绝对生物利用度仅为26%。与环糊精(CD)的包合络合已被报道可以增加各种化合物的水溶性。目的:通过与2-羟丙基-β-环糊精(HP-β-CD)包合提高OLM的口服生物利用度。材料与方法:采用物理混合和揉制两种方法制备HP-β-CD包合物。对所制备的配合物进行了药物含量、水溶性、溶出度、体外扩散、肠通透性和稳定性等指标的表征。用差示扫描量热法、x射线衍射法和傅里叶变换红外光谱法证实了包合物的形成。结果:所制配合物的溶解度、溶出度、扩散速率和肠通透性均明显高于普通药物。在形成包合物的两种方法中,KN法具有更高的溶解率,因此与PM相比是一种更好的方法。结论:该方法有望提高OLM的口服生物利用度。
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Studies on inclusion complex as potential systems for enhancement of oral bioavailability of olmesartan medoxomil
Background: Olmesartan medoxomil (OLM), an anti-hypertensive agent administered orally, has absolute bioavailability of only 26% due to the poor aqueous solubility (7.75 μg/ml). Inclusion complexation with cyclodextrins (CD) has been reported to increase the aqueous solubility of various compounds. Aim: The present investigation aimed to enhancing the oral bioavailability of OLM by inclusion complexation with 2-hydroxypropyl-β-cyclodextrin (HP-β-CD). Materials and Methods: The inclusion complexes with HP-β-CD were prepared using two different methods, viz., physical mixture and kneading. The prepared complexes were characterized for various parameters such as drug content, aqueous solubility, dissolution study, in vitro diffusion, intestinal permeability and stability study. The formation of the inclusion complex was confirmed by differential scanning calorimetry, X-ray diffraction, and Fourier transform infrared spectroscopy. Results: The solubility, dissolution, diffusion rate, and intestinal permeability of the prepared complexes were found to be significantly higher than that of the plain drug. Among the two methods used for formation of inclusion complex, KN method gave higher solubility rates and hence is a better method when compared with PM. Conclusion: The approach seems to be promising in improving the oral bioavailability of OLM.
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