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基于酶/ROS 双重敏感纳米平台的光诱导型 EGFR 抑制剂特异性释放用于非小细胞肺癌的分子靶向光动力联合治疗。

Photo-induced specific intracellular release EGFR inhibitor from enzyme/ROS-dual sensitive nano-platforms for molecular targeted-photodynamic combinational therapy of non-small cell lung cancer.

机构信息

School of Chemical Engineering, Sichuan University, Chengdu 610065, China.

出版信息

J Mater Chem B. 2020 Sep 21;8(35):7931-7940. doi: 10.1039/d0tb01053g. Epub 2020 Aug 11.

DOI:10.1039/d0tb01053g
PMID:32779670
Abstract

Molecular targeted-photodynamic combinational therapy is a promising strategy to enhance antitumor effects; meanwhile, current nanocarriers face challenges of limited selective delivery and release of therapeutic agents to specific tumor sites, which significantly compromises their therapeutic efficacy. Herein, we report active-targeting, enzyme- and ROS-dual responsive nanoparticles (HPGBCA) consisting of CD-targeting hyaluronic acid (HA) shells and afatinib (AFT)-loaded, ROS-sensitive poly(l-lysine)-conjugated chlorin e6 (Ce6) derivative nanoparticle cores (PGBCA). HPGBCA can actively carry AFT and Ce6 specifically to tumor cells due to the negatively charged HA and CD-mediated active targeting. Subsequently, hyaluronidase in the endosome will further spur the degradation of the HA shell to prompt exposure of the positively charged PGBCA core for rapid endosomal escape and intracellular delivery of AFT and Ce6. Furthermore, the generation of ROS produced by Ce6 under NIR irradiation can trigger the rapid oxidation of the thioether linker to facilitate the release of AFT into the cytoplasm. In vitro and in vivo studies demonstrated that the released AFT and excessive ROS at the local site can synergistically induce cell apoptosis to enhance the therapeutic efficacy without side effects. Our developed intelligent nanoparticle provides new avenues to achieve on-demand, specific intracellular drug release for improved molecular targeted-photodynamic combination therapeutic efficacy.

摘要

分子靶向-光动力联合治疗是增强抗肿瘤效果的一种很有前途的策略;同时,目前的纳米载体面临着治疗剂向特定肿瘤部位的有限选择性递送和释放的挑战,这大大降低了它们的治疗效果。在这里,我们报告了由靶向 CD 的透明质酸(HA)壳和载有阿法替尼(AFT)的、ROS 敏感的聚(L-赖氨酸)-接枝氯乙啶 6(Ce6)衍生物纳米颗粒核心(PGBCA)组成的主动靶向、酶和 ROS 双重响应的纳米颗粒(HPGBCA)。由于带负电荷的 HA 和 CD 介导的主动靶向,HPGBCA 可以主动携带 AFT 和 Ce6 特异性地靶向肿瘤细胞。随后,内体中的透明质酸酶将进一步促进 HA 壳的降解,以促使带正电荷的 PGBCA 核快速从内体逃逸和细胞内递送 AFT 和 Ce6。此外,Ce6 在近红外辐射下产生的 ROS 可以触发硫醚键的快速氧化,促进 AFT 释放到细胞质中。体外和体内研究表明,局部释放的 AFT 和过量的 ROS 可以协同诱导细胞凋亡,增强治疗效果,而没有副作用。我们开发的智能纳米颗粒为实现按需、特异性的细胞内药物释放提供了新途径,以提高分子靶向-光动力联合治疗的效果。

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Photo-induced specific intracellular release EGFR inhibitor from enzyme/ROS-dual sensitive nano-platforms for molecular targeted-photodynamic combinational therapy of non-small cell lung cancer.基于酶/ROS 双重敏感纳米平台的光诱导型 EGFR 抑制剂特异性释放用于非小细胞肺癌的分子靶向光动力联合治疗。
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