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首页> 外文期刊>International Journal of Nanomedicine >Near-infrared light-triggered theranostics for tumor-specific enhanced multimodal imaging and photothermal therapy
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Near-infrared light-triggered theranostics for tumor-specific enhanced multimodal imaging and photothermal therapy

机译:近红外光触发治疗学,用于肿瘤特异性增强型多模态成像和光热疗法

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The major challenge in current clinic contrast agents (CAs) and chemotherapy is the poor tumor selectivity and response. Based on the self-quench property of IR820 at high concentrations, and different contrast effect ability of Gd-DOTA between inner and outer of liposome, we developed “bomb-like” light-triggered CAs (LTCAs) for enhanced CT/MRI/FI multimodal imaging, which can improve the signal-to-noise ratio of tumor tissue specifically. IR820, Iohexol and Gd-chelates were firstly encapsulated into the thermal-sensitive nanocarrier with a high concentration. This will result in protection and fluorescence quenching. Then, the release of CAs was triggered by near-infrared (NIR) light laser irradiation, which will lead to fluorescence and MRI activation and enable imaging of inflammation. In vitro and in vivo experiments demonstrated that LTCAs with 808?nm laser irradiation have shorter T1 relaxation time in MRI and stronger intensity in FI compared to those without irradiation. Additionally, due to the high photothermal conversion efficiency of IR820, the injection of LTCAs was demonstrated to completely inhibit C6 tumor growth in nude mice up to 17 days after NIR laser irradiation. The results indicate that the LTCAs can serve as a promising platform for NIR-activated multimodal imaging and photothermal therapy.
机译:当前临床对比剂(CA)和化学疗法的主要挑战是差的肿瘤选择性和反应性。基于高浓度IR820的自猝灭特性,以及脂质体内部和外部之间Gd-DOTA的不同对比作用能力,我们开发了“炸弹状”光触发CA(LTCA)以增强CT / MRI / FI多模态成像,可以特别提高肿瘤组织的信噪比。首先将IR820,碘海醇和Gd螯合物以高浓度封装到热敏纳米载体中。这将导致保护和荧光猝灭。然后,CA的释放是由近红外(NIR)激光照射触发的,这将导致荧光和MRI激活,并使炎症成像成为可能。体外和体内实验表明,与未辐照相比,采用808?nm激光辐照的LTCA在MRI中具有更短的T 1 弛豫时间和更强的FI强度。此外,由于IR820的高光热转换效率,LTCAs的注射被证明可以完全抑制NIR激光照射后长达17天的C6肿瘤在裸鼠中的生长。结果表明,LTCAs可以作为近红外激活多峰成像和光热疗法的有前途的平台。

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