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一种具有三重刺激响应的双靶向透明质酸-金纳米棒平台,用于乳腺癌的光动力/光热治疗。

A dual-targeted hyaluronic acid-gold nanorod platform with triple-stimuli responsiveness for photodynamic/photothermal therapy of breast cancer.

机构信息

State Key Laboratory for Mechanical Behavior of Materials, Xi'an Jiaotong University, Xi'an 710049, China.

State Key Laboratory for Mechanical Behavior of Materials, Xi'an Jiaotong University, Xi'an 710049, China.

出版信息

Acta Biomater. 2019 Jan 1;83:400-413. doi: 10.1016/j.actbio.2018.11.026. Epub 2018 Nov 19.

Abstract

Multi-stimuli-responsive theranostic nanoplatform integrating functions of both imaging and multimodal therapeutics holds great promise for improving diagnosis and therapeutic efficacy. In this study, we reported a pH, glutathione (GSH) and hyaluronidase (HAase) triple-responsive nanoplatform for HER2 and CD44 dual-targeted and fluorescence imaging-guided PDT/PTT dual-therapy against HER2-overexpressed breast cancer. The nanoplatform was fabricated by functionalizing gold nanorods (GNRs) with hyaluronic acid (HA) bearing pendant hydrazide and thiol groups via Au-S bonds, and subsequently chemically conjugating 5-aminolevulinic acid (ALA), Cy7.5 and anti-HER2 antibody onto HA moiety for PDT, fluorescence imaging and active targeting, respectively. The resulting versatile nanoplatform GNR-HA-HER2 had uniform sizes, favorable dispersibility, as well as pH, GSH and HAase triple-responsive drug release manner. In vitro studies demonstrated that HER2 and CD44 receptor-mediated dual-targeting strategy could significantly enhance the cellular uptake of GNR-HA-HER2. Under near-infrared (NIR) irradiation, MCF-7 cells could efficiently generate reactive oxygen species (ROS) and heat, and be more efficiently killed by a combination of PDT and PTT as compared with individual therapy. Pharmacokinetic and biodistribution studies showed that the nanoplatform possessed a circulation half-life of 1.9 h and could be specifically delivered to tumor tissues with an accumulation ratio of 12.8%. Upon the fluorescence imaging-guided PDT/PTT treatments, the tumors were completely eliminated without obvious side effects. The results suggest that the GNR-HA-HER2 holds great potential for breast cancer therapy. STATEMENT OF SIGNIFICANCE: A combination of photodynamic therapy (PDT) and photothermal therapy (PTT) is emerging as a promising cancer treatment strategy. However, its therapeutic efficacy is compromised by the nonspecific delivery and unintended release of photo-responsive agents. Herein, we developed a multifunctional theranostic nanoplatform GNR-HA-HER2 with pH, glutathione and hyaluronidase triple-responsive drug release for HER2 and CD44 dual-targeted and fluorescence imaging-guided PDT/PTT therapy against breast cancer. We demonstrated that HER2 and CD44 receptors-mediated dual-targeting strategy significantly enhanced the cellular uptake of GNR-HA-HER2. We also demonstrated that the combined PDT/PTT treatment had significantly superior antitumor effect than PDT or PTT alone both in vitro and in vivo. Therefore, GNR-HA-HER2 could serve as a promising nanoplatform for HER2-positive breast cancer therapy.

摘要

多刺激响应治疗纳米平台集成了成像和多种治疗的功能,为提高诊断和治疗效果提供了巨大的前景。在本研究中,我们报道了一种 pH、谷胱甘肽 (GSH) 和透明质酸酶 (HAase) 三重响应的纳米平台,用于 HER2 和 CD44 双重靶向和荧光成像引导的 PDT/PTT 双重治疗过表达 HER2 的乳腺癌。该纳米平台是通过在金纳米棒 (GNRs) 上功能化具有侧接腙和巯基的透明质酸 (HA),通过 Au-S 键,随后将 5-氨基酮戊酸 (ALA)、Cy7.5 和抗 HER2 抗体化学偶联到 HA 部分用于 PDT、荧光成像和主动靶向,分别。所得多功能纳米平台 GNR-HA-HER2 具有均匀的尺寸、良好的分散性以及 pH、GSH 和 HAase 三重响应的药物释放方式。体外研究表明,HER2 和 CD44 受体介导的双重靶向策略可显著增强 GNR-HA-HER2 的细胞摄取。在近红外 (NIR) 照射下,与单独治疗相比,MCF-7 细胞可以更有效地产生活性氧 (ROS) 和热量,并通过 PDT 和 PTT 的组合更有效地杀死。药代动力学和生物分布研究表明,该纳米平台具有 1.9 h 的循环半衰期,并可特异性递送至肿瘤组织,其积累比为 12.8%。在荧光成像引导的 PDT/PTT 治疗下,肿瘤完全消除,无明显副作用。结果表明,GNR-HA-HER2 具有治疗乳腺癌的巨大潜力。

意义声明

光动力疗法 (PDT) 和光热疗法 (PTT) 的联合治疗正在成为一种很有前途的癌症治疗策略。然而,其治疗效果受到光响应性药物的非特异性传递和意外释放的影响。在此,我们开发了一种具有 pH、谷胱甘肽和透明质酸酶三重响应性药物释放的多功能治疗纳米平台 GNR-HA-HER2,用于 HER2 和 CD44 双重靶向和荧光成像引导的 PDT/PTT 治疗乳腺癌。我们证明了 HER2 和 CD44 受体介导的双重靶向策略显著增强了 GNR-HA-HER2 的细胞摄取。我们还证明,与单独的 PDT 或 PTT 相比,联合 PDT/PTT 治疗在体外和体内均具有显著优越的抗肿瘤效果。因此,GNR-HA-HER2 可作为一种有前途的 HER2 阳性乳腺癌治疗的纳米平台。

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