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Lipid-Based Nanoparticulate Systems for the Delivery of Anti-Cancer Drug Cock-

机译:基于脂质的纳米颗粒系统用于抗癌药物-

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摘要

The use of drug cocktails has become a widely adopted strategy in clinical cancer therapy. Cytotoxic drug cocktails are often administered based on maximum tolerated dose (MTD) of each agent, with the belief of achieving maximum cell kill through tolerable toxicity level. Yet, MTD administration may not have fully captured the therapeutic synergism that exists among the individual agents in the drug cocktail, as the response to a cocktail regimen, that is, whether the effect is synergistic or not, could be highly sensitive to the concentration ratios of the individual drugs at the site of action. It is important to realize that the inherently different pharmacokinetic profiles of the individual agents could have significant influence on the response to an anti-cancer drug cocktail by dictating the amount of the individual agents reaching the tumor site and therefore the concentration ratios. Furthermore, the individual agents may have unfavorable pharmacokinetic interactions that add to the difficulty in determining the therapeutic and/or toxicological effects of the drug cocktail. In this review, we will focus on how lipid-based nanoparticulate systems could address the above issues associated with anticancer drug cocktails. Specifically, we will highlight the use of liposome systems as the means to control and coordinate the delivery of various anti-cancer drug cocktails, encompassing conventional chemotherapeutics, chemosensitizing agents and molecularly targeted agents.
机译:药物鸡尾酒的使用已成为临床癌症治疗中被广泛采用的策略。通常根据每种药物的最大耐受剂量(MTD)来施用细胞毒性药物混合物,并相信可以通过耐受的毒性水平实现最大的细胞杀伤率。但是,MTD给药可能尚未完全捕捉到药物鸡尾酒中各个药物之间存在的治疗协同作用,因为对鸡尾酒疗法的反应(即效果是否协同)可能对浓度比高度敏感作用部位上的每种药物。重要的是要认识到,通过指示到达肿瘤部位的各个药剂的量以及浓度比,各个药剂的固有不同的药代动力学特性可能会对抗癌药混合物的反应产生重大影响。此外,各个试剂可能具有不利的药代动力学相互作用,这增加了确定药物混合物的治疗和/或毒理作用的难度。在这篇综述中,我们将重点研究基于脂质的纳米颗粒系统如何解决与抗癌药物混合物相关的上述问题。具体而言,我们将重点介绍使用脂质体系统作为控制和协调各种抗癌药混合物的传递的手段,包括传统的化学治疗剂,化学增敏剂和分子靶向剂。

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