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基于近红外石墨烯量子点的稀土纳米颗粒介导的线粒体靶向光动力疗法。

Mitochondrial specific photodynamic therapy by rare-earth nanoparticles mediated near-infrared graphene quantum dots.

机构信息

MOE Key Laboratory of Laser Life Science and Institute of Laser Life Science, College of Biophotonics, South China Normal University, Guangzhou 510631, PR China.

MOE Key Laboratory of Laser Life Science and Institute of Laser Life Science, College of Biophotonics, South China Normal University, Guangzhou 510631, PR China.

出版信息

Biomaterials. 2018 Jan;153:14-26. doi: 10.1016/j.biomaterials.2017.10.034. Epub 2017 Oct 23.

DOI:10.1016/j.biomaterials.2017.10.034
PMID:29096398
Abstract

Photodynamic therapy (PDT) has been proposed in cancer treatment for decades, but its clinical translation is significantly impeded by the low yield of ROS, poor tissue penetration depth of most current photosensitizers, and short lifetime of ROS. These limitations directly affect the therapeutic effect of PDT in cancer therapy. Here we proposed a new strategy by collaboratively integrating rare-earth doped upconversion nanoparticles (UCNP) with graphene quantum dot (GQD) for highly efficacious PDT, based on the merits of UCNP, which can emit UV-vis light under near-infrared light (NIR) excitation, and GQD, which can produce O efficiently. For GQD-decorated UCNP nanoparticles (UCNP-GQD), the emission light from UCNP can further excite GQD with prominent O generation for NIR-triggered PDT. Furthermore, a hydrophilic rhodamine derivative, TRITC, is covalently tethered to afford the resultant UCNP-GQD/TRITC, possessing distinct mitochondrial targeting property. Thus mitochondrial specific PDT with in-situO burst in mitochondria induces sharp decrease of mitochondrial membrane potential, which initiates the tumor cell apoptosis irreversibly. Importantly, in vivo experiments demonstrate the tumor inhibition of mitochondrial targeting UCNP-GQD/TRITC with improved therapeutic efficiency compared with non-targeting UCNP-GQD. The proposed strategy highlights the advantages of precision organelles-specific PDT in cancer therapy.

摘要

光动力疗法(PDT)在癌症治疗中已经提出了几十年,但由于 ROS 产量低、大多数现有光敏剂的组织穿透深度差以及 ROS 的寿命短,其临床转化受到了显著阻碍。这些限制直接影响 PDT 在癌症治疗中的治疗效果。在这里,我们提出了一种新的策略,通过协同整合稀土掺杂上转换纳米粒子(UCNP)与石墨烯量子点(GQD),以实现高效的 PDT,这一策略基于 UCNP 的优点,即在近红外光(NIR)激发下可以发射 UV-vis 光,以及 GQD 的优点,即可以高效地产生 O。对于 GQD 修饰的 UCNP 纳米粒子(UCNP-GQD),UCNP 的发射光可以进一步激发 GQD,产生显著的 O 生成,用于 NIR 触发的 PDT。此外,亲水性罗丹明衍生物 TRITC 通过共价键连接到 UCNP-GQD 上,赋予其固有的线粒体靶向特性。因此,线粒体特异性 PDT 可以在线粒体中引发原位 O 爆发,导致线粒体膜电位急剧下降,从而不可逆地引发肿瘤细胞凋亡。重要的是,体内实验表明,与非靶向 UCNP-GQD 相比,具有线粒体靶向性的 UCNP-GQD/TRITC 具有更好的治疗效果,抑制了肿瘤的生长。该策略突出了精准细胞器特异性 PDT 在癌症治疗中的优势。

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