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基于纳米载体的免疫/化学联合递药双重区域选择性靶向同一受体以增强影像引导癌症治疗

Dual Regioselective Targeting the Same Receptor in Nanoparticle-Mediated Combination Immuno/Chemotherapy for Enhanced Image-Guided Cancer Treatment.

机构信息

Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, 16/10 Miklukho-Maklaya Street, Moscow 117997, Russia.

MEPhI (Moscow Engineering Physics Institute), Institute of Engineering Physics for Biomedicine (PhysBio), 31 Kashirskoe Shosse, Moscow 115409, Russia.

出版信息

ACS Nano. 2020 Oct 27;14(10):12781-12795. doi: 10.1021/acsnano.0c03421. Epub 2020 Sep 16.

DOI:10.1021/acsnano.0c03421
PMID:32935975
Abstract

When combined with immunotherapy, image-guided targeted delivery of chemotherapeutic agents is a promising direction for combination cancer theranostics, but this approach has so far produced only limited success due to a lack of molecular targets on the cell surface and low therapeutic index of conventional chemotherapy drugs. Here, we demonstrate a synergistic strategy of combination immuno/chemotherapy in conditions of dual regioselective targeting, implying vectoring of two distinct binding sites of a single oncomarker (here, HER2) with theranostic compounds having a different mechanism of action. We use: (i) PLGA nanoformulation, loaded with an imaging diagnostic fluorescent dye (Nile Red) and a chemotherapeutic drug (doxorubicin), and functionalized with affibody Z (8 kDa); (ii) bifunctional genetically engineered DARP-LoPE (42 kDa) immunotoxin comprising of a low-immunogenic modification of therapeutic exotoxin A (LoPE) and a scaffold targeting protein, DARPin9.29 (14 kDa). According to the proposed strategy, the first chemotherapeutic nanoagent is targeted by the affibody to subdomain III and IV of HER2 with 60-fold specificity compared with nontargeted particles, while the second immunotoxin is effectively targeted by DARPin molecule to subdomain I of HER2. We demonstrate that this dual targeting strategy can enhance anticancer therapy of HER2-positive cells with a very strong synergy, which made possible 1000-fold decrease of effective drug concentration and a significant enhancement of HER2 cancer therapy compared to monotherapy . Moreover, this therapeutic combination prevented the appearance of secondary tumor nodes. Thus, the suggested synergistic strategy utilizing dual targeting of the same oncomarker could give rise to efficient methods for aggressive tumors treatment.

摘要

当与免疫疗法结合时,基于图像引导的靶向递药系统联合化疗是癌症联合治疗的一个很有前途的方向,但由于细胞表面缺乏分子靶点和传统化疗药物的治疗指数低,这种方法迄今为止只取得了有限的成功。在这里,我们展示了一种联合免疫/化疗的协同策略,即在双重区域选择性靶向的条件下,利用单一肿瘤标志物(这里是 HER2)的两个不同结合位点与具有不同作用机制的治疗化合物相结合。我们使用:(i)载有成像诊断荧光染料(Nile Red)和化疗药物(阿霉素)的 PLGA 纳米制剂,并与具有不同作用机制的治疗化合物相结合,同时具有亲和力 Z(8 kDa);(ii)双功能基因工程 DARP-LoPE(42 kDa)免疫毒素,由低免疫原性修饰的治疗性外毒素 A(LoPE)和靶向蛋白 DARPin9.29(14 kDa)组成。根据所提出的策略,第一个化疗纳米药物通过亲和力 Z 靶向 HER2 的亚结构域 III 和 IV,与非靶向颗粒相比具有 60 倍的特异性,而第二个免疫毒素则通过 DARPin 分子有效地靶向 HER2 的亚结构域 I。我们证明,这种双重靶向策略可以增强 HER2 阳性细胞的抗癌治疗效果,具有很强的协同作用,使有效药物浓度降低 1000 倍,并显著增强 HER2 癌症治疗效果,优于单药治疗。此外,这种治疗组合还可以防止继发性肿瘤节点的出现。因此,建议的利用相同肿瘤标志物的双重靶向协同策略可能为侵袭性肿瘤的治疗提供有效的方法。

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