Review of current trends in enhancing bioavailability of poorly water soluble drugs by liposomal interventions

S. Majekodunmi
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引用次数: 1

Abstract

One of the several ways of enhancing the solubility of poorly soluble drugs is liposomes formulations. Research on liposomes formulations has progressed from that of conventional vesicles to new generation liposomes, such as cationic liposomes, temperature sensitive liposomes, and virosomes, by modulating the formulation techniques and lipid composition. Thermosensitive liposomes are also a promising tool for external targeting of drugs to solid tumors when used in combination with local hyperthermia or high intensity focused ultrasound. In vivo results have demonstrated strong evidence that external targeting is superior over passive targeting achieved by highly stable long-circulating drug formulations like PEGylated liposomal doxorubicin. This review is to compare the therapeutic effect of current clinically approved liposomebased drugs with free drugs and summarize the historical development and effects of particular phospholipids and surfactants on the biophysical properties and in vivo efficacy of thermosensitive liposome formulations. Drug delivery guided by magnetic resonance imaging is also discussed. The combination of external targeting with thermosensitive liposomes and magnetic resonance-guided drug delivery will be the unique characteristics of this nanotechnology approach in medicine.
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通过脂质体干预提高难水溶性药物生物利用度的当前趋势综述
提高难溶性药物溶解度的几种方法之一是脂质体制剂。脂质体的剂型研究已从传统的囊泡剂型发展到阳离子型脂质体、温敏型脂质体、病毒体等新一代脂质体。当与局部热疗或高强度聚焦超声联合使用时,热敏脂质体也是一种很有前景的药物外部靶向实体肿瘤的工具。体内实验结果有力地证明,外部靶向优于高度稳定的长循环药物制剂(如聚乙二醇化脂质体阿霉素)的被动靶向。本文对目前临床批准的基于脂质体的药物与游离药物的治疗效果进行了比较,并对某些磷脂和表面活性剂对热敏性脂质体制剂的生物物理性质和体内疗效的历史发展和影响进行了综述。还讨论了磁共振成像引导给药的方法。体外靶向与热敏脂质体和磁共振引导给药的结合将是这种纳米技术在医学上的独特特点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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