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用于极低近红外激活光热治疗的核靶向金纳米棒。

Nuclear-Targeting Gold Nanorods for Extremely Low NIR Activated Photothermal Therapy.

机构信息

State Key Laboratory of High Performance Ceramics and Superfine Microstructure, Shanghai Institute of Ceramics, Chinese Academy of Sciences , 1295 Ding-Xi Road, Shanghai 200050, China.

出版信息

ACS Appl Mater Interfaces. 2017 May 17;9(19):15952-15961. doi: 10.1021/acsami.7b03017. Epub 2017 May 3.

Abstract

Photorelated nanomedicine is of particular interest as an emerging paradigm toward precise cancer therapy, as demonstrated by recent developments of photothermal therapy (PTT), an emerging technique employing light-converting agents to burn cancerous cells by overdosed optical energy-converted heat. However, most of the laser irradiations needed for effective PTT significantly exceed the maximal permissible power density in human skin, which is likely to damage surrounding normal tissues. Herein, we report a strategy of intranuclear PTT of cancer enabled by nuclear-targeted delivery of gold nanorods of ∼10.5 × 40.5 nm in size via conjugation with nuclear location signal peptides (GNRs-NLS) under an extremely low near-infrared irradiation of 0.2 W/cm, much below the maximal permissible exposure of skin. Interestingly, we found that a mild but nuclear-focused temperature increase generated by GNRs-NLS is sufficient to cause damage to intranuclear DNA and the inhibition of DNA repair process, which, interestingly, led to the cancer cell apoptosis rather than to conventional cell necrosis by thermal ablation during PTT. Correspondingly, tumors treated with GNRs-NLS exhibited gradual but significant regressions rather than traditional harsh burning-up of tumors, in comparison with negligible antitumor effect by GNRs without nuclear targeting under the same ultralow NIR irradiation. This report demonstrates the successful intranuclear efficient photothermal therapy of cancer via cell apoptosis by photoadsorbing agents, e.g., GNRs-NLS in the present case, with largely mitigated side-effect on normal tissues and therefore substantially improved biosafety.

摘要

光相关纳米医学作为一种精确癌症治疗的新兴范例引起了特别的关注,这一点已被光热疗法(PTT)的最新发展所证明,PTT 是一种新兴技术,它利用光转化剂将过量的光能量转化为热能来燃烧癌细胞。然而,大多数有效 PTT 所需的激光辐照显著超过了人类皮肤的最大允许功率密度,这可能会损伤周围的正常组织。在此,我们通过将大小约为 10.5×40.5nm 的金纳米棒与核定位信号肽(GNRs-NLS)缀合,报告了一种通过核靶向递送来实现癌症的核内 PTT 的策略,这种方法在 0.2 W/cm 的极低近红外照射下实现,远低于皮肤的最大允许暴露量。有趣的是,我们发现,GNRs-NLS 产生的温和但聚焦于核的温度升高足以导致核内 DNA 损伤和 DNA 修复过程的抑制,有趣的是,这导致了癌细胞凋亡,而不是通过 PTT 中的热烧蚀导致常规的细胞坏死。相应地,与没有核靶向的 GNRs 在相同的超低近红外照射下几乎没有抗肿瘤作用相比,用 GNRs-NLS 治疗的肿瘤表现出逐渐但显著的消退,而不是传统的肿瘤强烈燃烧。本报告通过光吸附剂(例如在本案例中的 GNRs-NLS)成功实现了癌症的核内高效光热疗法,通过细胞凋亡,对正常组织的副作用大大减轻,因此生物安全性得到了极大提高。

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