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靶向肿瘤相关纤维连接蛋白的 aptide-多西他赛偶联物的合成与治疗评估。

Synthesis and therapeutic evaluation of an aptide-docetaxel conjugate targeting tumor-associated fibronectin.

机构信息

School of Life Sciences, Gwangju Institute of Science and Technology, 123 Cheomdangwagi-ro, Gwangju 500-712, Republic of Korea.

KAIST Institute for the BioCentury, Department of Biological Sciences, Korea Advanced Institute of Science and Technology, 291 Daehak-ro, Daejeon 305-701, Republic of Korea.

出版信息

J Control Release. 2014 Mar 28;178:118-24. doi: 10.1016/j.jconrel.2014.01.015. Epub 2014 Jan 23.

DOI:10.1016/j.jconrel.2014.01.015
PMID:24462899
Abstract

Targeted delivery of anticancer drugs to tumors has attracted considerable research interest because of its potential to reduce adverse toxicity while improving therapeutic efficacy. In this study, we synthesized and evaluated the therapeutic efficacy of a conjugate of a high-affinity peptide (aptide) and the anticancer drug docetaxel (DTX). A fibronectin extra domain B (EDB)-specific aptide (APTEDB) was used as a cancer-specific targeting ligand. An APTEDB-DTX conjugate was synthesized from an alkyne-modified aptide and azide-modified DTX via click chemistry. A microscopy study revealed selective binding of dye-labeled APTEDB to EDB-overexpressing cancer cells. The cytotoxicity of the conjugate toward EDB-overexpressing murine lung carcinoma (LLC) and human glioblastoma (U87MG) was similar to that of free DTX. In a pharmacokinetic study, APTEDB-DTX formulated with PEG400/ethanol(5%) exhibited a circulation half-life similar to that of a Tween-80/ethanol formulation of parent DTX. Finally, an evaluation of intravenously injected APTEDB-DTX in mice bearing EDB-positive tumors showed that APTEDB-DTX inhibited the growth of both LLC allograft and U87MG xenograft tumors with an efficacy better than the parent-DTX formulation but with much lower toxicity, as evidenced by reduced body weight loss. Taken together, these results indicate that the aptide-drug conjugate system described here may hold potential as a targeted therapy regimen.

摘要

靶向递送至肿瘤的抗癌药物引起了相当多的研究兴趣,因为它有可能降低不良反应毒性,同时提高治疗效果。在这项研究中,我们合成并评估了高亲和力肽(aptide)和抗癌药物多西紫杉醇(DTX)缀合物的治疗效果。纤连蛋白外域 B(EDB)特异性 aptide(APTEDB)被用作癌症特异性靶向配体。通过点击化学,将炔基修饰的 aptide 和叠氮化物修饰的 DTX 合成 APTEDB-DTX 缀合物。显微镜研究表明,染料标记的 APTEDB 选择性结合于 EDB 过表达的癌细胞。缀合物对 EDB 过表达的小鼠肺癌(LLC)和人神经胶质瘤(U87MG)的细胞毒性与游离 DTX 相似。在药代动力学研究中,用 PEG400/乙醇(5%)配制的 APTEDB-DTX 表现出与 Tween-80/乙醇制剂的母体 DTX 相似的循环半衰期。最后,在携带 EDB 阳性肿瘤的小鼠中评估静脉注射的 APTEDB-DTX 表明,与母体-DTX 制剂相比,APTEDB-DTX 抑制 LLC 同种异体移植瘤和 U87MG 异种移植瘤的生长,效果更好,但毒性降低,体重减轻减轻。综上所述,这些结果表明,本文描述的 aptide-药物缀合物系统可能具有作为靶向治疗方案的潜力。

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