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In vivo targeted deep-tissue photodynamic therapy based on near-infrared light triggered upconversion nanoconstruct

机译:基于近红外光触发的上转换纳米结构的体内靶向深层组织光动力疗法

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摘要

Two major challenges of current photodynamic therapy (PDT) are the limited tissue penetration of excitation light and poor tumor-selectivity of the photosensitizer (PS). To address these issues, we developed a multifunctional nanoconstruct consisting of upconversion nanoparticles (UCNPs) that transform near-infrared (NIR) light to visible light and a photosensitizer zinc(II) phthalocyanine (ZnPc). Folate-modified amphiphilic chitosan (FASOC) was coated on the surface of UCNPs to anchor the ZnPc close to the UCNPs, thereby facilitating resonance energy transfer from UCNPs to ZnPc. Confocal microscopy and NIR small animal imaging demonstrated the enhanced tumor-selectivity of the nanoconstructs to cancer cells that overexpressed folate receptor. Reactive oxygen species (ROS) generation in cancer cells under a 1-cm tissue was higher upon excitation of UCNPs with the 980 nm light than that with 660 nm irradiation. In vivo PDT treatments for deep-seated tumors demonstrated that NIR light-triggered PDT based on the nanoconstructs possessed remarkable therapeutic efficacy with tumor inhibition ratio up to 50% compared with conventional visible light-activated PDT with a noticeable reduced tumor inhibition ratio of 18%. These results indicate that the multifunctional nanoconstruct is a promising PDT agent for deep-seated tumor treatment and demonstrate a new paradigm for enhancing PDT efficacy.
机译:当前的光动力疗法(PDT)的两个主要挑战是激发光的组织渗透受限和光敏剂(PS)的不良肿瘤选择性。为了解决这些问题,我们开发了一种多功能纳米结构,该结构由将近红外(NIR)光转换为可见光的上转换纳米颗粒(UCNP)和光敏剂酞菁锌(II)组成。将叶酸修饰的两亲性壳聚糖(FASOC)涂覆在UCNPs的表面上,以将ZnPc锚定在UCNPs附近,从而促进从UCNPs到ZnPc的共振能量转移。共聚焦显微镜和NIR小动物成像表明,纳米结构对过表达叶酸受体的癌细胞具有更高的肿瘤选择性。用980 nm的光激发UCNP后,在1 cm组织下癌细胞中的活性氧(ROS)生成要高于用660 nm的辐射。体内PDT对深层肿瘤的治疗表明,基于NIR的NIR光触发PDT具有显着的治疗效果,与传统的可见光激活PDT相比,其肿瘤抑制率高达50%,显着降低的肿瘤抑制率达18% 。这些结果表明,多功能纳米构造物是用于深层肿瘤治疗的有前途的PDT剂,并证明了增强PDT功效的新范例。

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