Liposomes as carriers of hydrophilic small molecule drugs: Strategies to enhance encapsulation and delivery

脂质体 药物输送 纳米技术 小分子 体内分布 Zeta电位 化学 药品 生物物理学 药理学 材料科学 纳米颗粒 体外 生物化学 医学 生物
作者
Josimar O. Eloy,Marina Claro de Souza,Raquel Petrilli,Juliana Palma Abriata Barcellos,Robert J. Lee,Juliana Maldonado Marchetti
出处
期刊:Colloids and Surfaces B: Biointerfaces [Elsevier]
卷期号:123: 345-363 被引量:412
标识
DOI:10.1016/j.colsurfb.2014.09.029
摘要

Although hydrophilic small molecule drugs are widely used in the clinic, their rapid clearance, suboptimal biodistribution, low intracellular absorption and toxicity can limit their therapeutic efficacy. These drawbacks can potentially be overcome by loading the drug into delivery systems, particularly liposomes; however, low encapsulation efficiency usually results. Many strategies are available to improve both the drug encapsulation efficiency and delivery to the target site to reduce side effects. For encapsulation, passive and active strategies are available. Passive strategies encompass the proper selection of the composition of the formulation, zeta potential, particle size and preparation method. Moreover, many weak acids and bases, such as doxorubicin, can be actively loaded with high efficiency. It is highly desirable that once the drug is encapsulated, it should be released preferentially at the target site, resulting in an optimal therapeutic effect devoid of side effects. For this purpose, targeted and triggered delivery approaches are available. The rapidly increasing knowledge of the many overexpressed biochemical makers in pathological sites, reviewed herein, has enabled the development of liposomes decorated with ligands for cell-surface receptors and active delivery. Furthermore, many liposomal formulations have been designed to actively release their content in response to specific stimuli, such as a pH decrease, heat, external alternating magnetic field, ultrasound or light. More than half a century after the discovery of liposomes, some hydrophilic small molecule drugs loaded in liposomes with high encapsulation efficiency are available on the market. However, targeted liposomes or formulations able to deliver the drug after a stimulus are not yet a reality in the clinic and are still awaited.
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