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近红外闪烁的治疗诊断纳米粒子的微流控合成:用于 X 射线诱导光动力治疗的下一代剂量测定法。

Microfluidic Synthesis of Theranostic Nanoparticles with Near-Infrared Scintillation: Toward Next-Generation Dosimetry in X-ray-Induced Photodynamic Therapy.

机构信息

Departamento de Física. FFCLRP- Universidade de São Paulo, Ribeirão Preto, SP 14040-901, Brazil.

出版信息

ACS Appl Mater Interfaces. 2022 Jan 12;14(1):324-336. doi: 10.1021/acsami.1c20689. Epub 2021 Dec 28.

Abstract

We developed a microfluidic synthesis to grow GdF:Eu theranostic scintillating nanoparticles to simultaneously monitor the X-ray dose delivered to tumors during treatments with X-ray activated photodynamic therapy (X-PDT). The flow reaction was optimized to enhance scintillation emission from the Eu ions. The as-prepared ∼15 nm rhombohedral-shaped nanoparticles self-assembled into ∼100 nm mesoporous flower-like nanostructures, but the rhombohedral units remained intact and the scintillation spectra unaltered. The conjugation of the ScNPs with multilayers of methylene blue (MB) in a core-shell structure (GdF@MB) resulted in enhanced singlet oxygen (O) generation under X-ray irradiation, with maximum O production for nanoparticles with 4 MB layers (GdF@4MB). High O yield was further evidenced in cytotoxicity assays, demonstrating complete cell death only for the association of ScNPs with MB and X-rays. Because the scintillating Eu emission at 694 nm is within the therapeutic window and was only partially absorbed by the MB molecules, it was explored for getting dosimetric information. Using porcine skin and fat to simulate the optical and radiological properties of the human tissues, we showed that the scintillation light can be detected for a tissue layer of ∼16 mm, thick enough to be employed in radiotherapy treatments of breast cancers, for instance. Therefore, the GdF:Eu ScNPs and the GdF@4MB nanoconjugates are strong candidates for treating cancer with X-PDT while monitoring the treatment and the radiation dose delivered, opening new avenues to develop a next-generation modality of real-time dosimetry.

摘要

我们开发了一种微流体制备方法来生长 GdF:Eu 治疗诊断闪烁纳米粒子,以在 X 射线激活光动力疗法(X-PDT)治疗期间同时监测肿瘤接受的 X 射线剂量。优化了流动反应以增强 Eu 离子的闪烁发射。所制备的 ∼15nm 三方晶系纳米粒子自组装成 ∼100nm 介孔花状纳米结构,但三方晶系单元保持完整,闪烁光谱不变。通过将 ScNPs 与多层亚甲基蓝(MB)进行核壳结构(GdF@MB)的偶联,导致在 X 射线照射下产生增强的单线态氧(O),其中具有 4 层 MB 的纳米粒子(GdF@4MB)产生最大的 O 产量。在细胞毒性测定中进一步证明了高 O 产量,仅对于 ScNPs 与 MB 和 X 射线的结合导致完全细胞死亡。由于在 694nm 处的闪烁 Eu 发射处于治疗窗口内,并且仅被 MB 分子部分吸收,因此研究了它以获取剂量信息。使用猪皮和脂肪模拟人体组织的光学和放射学特性,我们表明可以检测到约 16mm 厚的组织层的闪烁光,足以用于例如乳腺癌的放射治疗。因此,GdF:Eu ScNPs 和 GdF@4MB 纳米复合物是 X-PDT 治疗癌症的理想候选物,同时可以监测治疗过程和辐射剂量,为开发下一代实时剂量学方法开辟了新途径。

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