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Hypoxia-triggered single molecule probe for high-contrast NIR II/PA tumor imaging and robust photothermal therapy

机译:低氧触发的单分子探针用于高对比度NIR II / PA肿瘤成像和强大的光热疗法

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摘要

Hypoxia is a common characteristic of solid tumors. This important feature is associated with resistance to radio-chemotherapy, which results in poor prognosis and probability of tumor recurrence. Taking advantage of background-free NIR II fluorescence imaging and deeper-penetrating photoacoustic (PA) imaging, we developed a hypoxia-triggered and nitroreductase (NTR) enzyme-responsive single molecule probe for high-contrast NIR II/PA tumor imaging and hypoxia-activated photothermal therapy (PTT), which will overcome cellular resistance during hypoxia.>Methods: The single molecule probe IR1048-MZ was synthesized by conjugating a nitro imidazole group as a specific hypoxia trigger with an IR-1048 dye as a NIR II/PA signal reporter. We investigated the NIR II fluorescence, NIR absorbance and photothermal effect in different hypoxia conditions in vitro, and performed NIR II/PA tumor imaging and hypoxia-activated photothermal therapy in mice.>Results: This versatile molecular probe IR1048-MZ not only realized high-contrast tumor visualization with a clear boundary by NIR II fluorescence imaging, but also afforded deep-tissue penetration at the centimeter level by 3D PA imaging. Moreover, after being activated by NTR that is overexpressed in hypoxic tumors, the probe exhibited a significant photothermal effect for curative tumor ablation with no recurrence.>Conclusions: We have developed the first hypoxia-triggered and NTR enzyme-responsive single molecule probe for high-contrast NIR II/PA tumor imaging and hypoxia-activated photothermal therapy. By tracing the activity of NTR, IR1048-MZ may be a promising contrast agent and theranostic formulation for other hypoxia-related diseases (such as cancer, inflammation, stroke, and cardiac ischemia).
机译:缺氧是实体瘤的共同特征。该重要特征与对放射化学疗法的抗性有关,这导致不良的预后和肿瘤复发的可能性。利用无背景的NIR II荧光成像和更深穿透的光声(PA)成像,我们开发了一种低氧触发和亚硝基还原酶(NTR)酶反应性单分子探针,用于高对比度NIR II / PA肿瘤成像和低氧-激活的光热疗法(PTT),可以克服缺氧时的细胞耐药性。>方法:通过将作为特定缺氧触发条件的硝基咪唑基团与IR-1048染料缀合来合成单分子探针IR1048-MZ作为NIR II / PA信号报告器。我们在体外研究了不同缺氧条件下的NIR II荧光,NIR吸收和光热效应,并在小鼠中进行了NIR II / PA肿瘤成像和低氧激活的光热疗法。>结果:这款多功能分子探针IR1048 -MZ不仅可以通过NIR II荧光成像实现清晰边界的高对比度肿瘤可视化,还可以通过3D PA成像在厘米水平上实现深层组织穿透。此外,在缺氧性肿瘤中过表达的NTR激活后,该探针对治愈性肿瘤的消融表现出了显着的光热作用,且没有复发。>结论:我们开发了第一个低氧触发的NTR酶,响应性单分子探针,用于高对比度NIR II / PA肿瘤成像和缺氧激活的光热疗法。通过追踪NTR的活性,IR1048-MZ可能成为其他缺氧相关疾病(如癌症,炎症,中风和心脏缺血)的有希望的造影剂和治疗学制剂。

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