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肿瘤治疗中基于微粒药物载体的主动靶向:基础与最新进展

Active targeting with particulate drug carriers in tumor therapy: fundamentals and recent progress.

作者信息

Marcucci Fabrizio, Lefoulon François

机构信息

Reparto di Epidemiologia Clinica, Istituto Superiore di Sanità, Viale Regina Elena 299, 00161 Rome, Italy.

出版信息

Drug Discov Today. 2004 Mar 1;9(5):219-28. doi: 10.1016/S1359-6446(03)02988-X.

DOI:10.1016/S1359-6446(03)02988-X
PMID:14980540
Abstract

Drug therapy for the treatment of tumors is often limited by a narrow therapeutic index. One approach that overcomes this limitation is the active targeting of tumors with particulate drug carriers. The derivatization of particulate drug carriers with a ligand leads to the selective targeting of the particulate to selected cells, thereby focusing drug delivery. In addition, particulate drug carriers have a high loading capacity, do not need covalent conjugation of the drug and the formulation protects the entrapped drug from enzymatic inactivation. Despite these favorable properties, their therapeutic efficacy in animal models has been reported only in recent years. The use of internalizing ligands and the targeting of intravascular tumor cells and endothelial cells of tumor blood vessels have been instrumental in demonstrating the clinical effectiveness of particulate drug carriers in animal models. As a result, several actively targeted particulate carriers have now entered, or are about to enter, clinical investigation. Recent findings, for example, the identification of cell-penetrating peptides with restricted cell selectivity, suggest that further improvements in this approach are likely in the near future.

摘要

肿瘤治疗的药物疗法常常受到治疗指数狭窄的限制。克服这一限制的一种方法是使用微粒药物载体对肿瘤进行主动靶向。用配体对微粒药物载体进行衍生化可导致微粒选择性靶向选定的细胞,从而实现药物递送的靶向性。此外,微粒药物载体具有高载药量,无需药物进行共价缀合,并且该制剂可保护包封的药物不被酶灭活。尽管具有这些有利特性,但它们在动物模型中的治疗效果直到近年来才被报道。使用内化配体以及靶向血管内肿瘤细胞和肿瘤血管的内皮细胞有助于证明微粒药物载体在动物模型中的临床有效性。因此,几种主动靶向的微粒载体现已进入或即将进入临床研究。例如,最近的研究发现,具有受限细胞选择性的细胞穿透肽的鉴定表明,在不久的将来这种方法可能会有进一步的改进。

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