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Limited Efficiency of Drug Delivery to Specific Intracellular Organelles Using Subcellularly 'Targeted' Drug Delivery Systems

机译:使用亚细胞“靶向”药物递送系统将药物递送至特定细胞内细胞器的效率有限

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Many drugs have been designed to act on intracellular targets and to affect intracellular processes inside target cells. For the desired effects to be exerted, these drugs should permeate target cells and reach specific intracellular organelles. This subcellular drug targeting approach has been proposed for enhancement of accumulation of these drugs in target organelles and improved efficiency. This approach is based on drug encapsulation in drug delivery systems (DDSs) and/or their decoration with specific targeting moieties that are intended to enhance the drug/DDS accumulation in the intracellular organelle of interest. During recent years, there has been a constant increase in interest in DDSs targeted to specific intracellular organelles, and many different approaches have been proposed for attaining efficient drug delivery to specific organelles of interest. However, it appears that in many studies insufficient efforts have been devoted to quantitative analysis of the major formulation parameters of the DDSs disposition (efficiency of DDS endocytosis and endosomal escape, intracellular trafficking, and efficiency of DDS delivery to the target organelle) and of the resulting pharmacological effects. Thus, in many cases, claims regarding efficient delivery of drug/DDS to a specific organelle and efficient subcellular targeting appear to be exaggerated. On the basis of the available experimental data, it appears that drugs/DDS decoration with specific targeting residues can affect their intracellular fate and result in preferential drug accumulation within an organelle of interest. However, it is not clear whether these approaches will be efficient in in vivo settings and be translated into preclinical and clinical applications. Studies that quantitatively assess the mechanisms, barriers, and efficiencies of subcellular drug delivery and of the associated toxic effects are required to determine the therapeutic potential of subcellular DDS targeting.
机译:已经设计了许多药物以作用于细胞内靶标并影响靶细胞内的细胞内过程。为了发挥所需的作用,这些药物应渗透靶细胞并到达特定的细胞内细胞器。已经提出了这种亚细胞药物靶向方法来增强这些药物在靶细胞器中的积累并提高效率。该方法基于药物递送系统(DDS)中的药物封装和/或它们具有特定靶向部分的修饰,这些靶向部分旨在增强药物/ DDS在感兴趣的细胞内细胞器中的积累。近年来,对靶向特定细胞内细胞器的DDS的兴趣一直在不断增加,并且已经提出了许多不同的方法来实现将药物有效地递送至感兴趣的特定细胞器。但是,似乎在许多研究中,都没有对DDS处置的主要配方参数(DDS内吞作用和内体逃逸的效率,细胞内贩运以及DDS输送至靶细胞的效率)的定量分析进行充分的努力。产生药理作用。因此,在许多情况下,关于将药物/ DDS有效递送至特定细胞器和有效亚细胞靶向的主张似乎被夸大了。根据可获得的实验数据,看来具有特定靶向残基的药物/ DDS修饰可影响其细胞内命运并导致感兴趣的细胞器内的优先药物蓄积。但是,尚不清楚这些方法在体内环境中是否有效,是否可以转化为临床前和临床应用。需要进行定量评估亚细胞药物递送的机制,障碍和效率以及相关毒性作用的研究,以确定亚细胞DDS靶向治疗的潜力。

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