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A pH-activatable and aniline-substituted photosensitizer for near-infrared cancer theranostics

机译:用于近红外癌症治疗的pH活化和苯胺取代的光敏剂

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摘要

This work reports a newly designed pH-activatable and aniline-substituted aza-boron-dipyrromethene as a trifunctional photosensitizer to achieve highly selective tumor imaging, efficient photodynamic therapy (PDT) and therapeutic self-monitoring through encapsulation in a cRGD-functionalized nanomicelle. The diethylaminophenyl is introduced in to the structure for pH-activatable near-infrared fluorescence and singlet oxygen (1O2) generation, and bromophenyl is imported to increase the 1O2 generation efficiency upon pH activation by virtue of its heavy atom effect. After encapsulation, the nanoprobe can target αvβ3 integrin-rich tumor cells via cRGD and is activated by physiologically acidic pH for cancer discrimination and PDT. The fascinating advantage of the nanoprobe is near-infrared implementation beyond 800 nm, which significantly improves the imaging sensitivity and increases the penetration depth of the PDT. By monitoring the fluorescence decrease in the tumor region after PDT, the therapeutic efficacy is demonstrated in situ and in real time, which provides a valuable and convenient self-feedback function for PDT efficacy tracking. Therefore, this rationally designed and carefully engineered nanoprobe offers a new paradigm for precise tumor theranostics and may provide novel opportunities for future clinical cancer treatment.
机译:这项工作报告了一种新设计的可pH活化和苯胺取代的氮杂硼-双-吡咯二烯,作为三功能光敏剂,可通过封装在cRGD功能化的纳米胶束中来实现高度选择性的肿瘤成像,有效的光动力疗法(PDT)和治疗性自我监测。将二乙氨基苯基引入结构中以产生pH活化的近红外荧光和单线态氧( 1 O2)生成,并引入溴苯以提高 1 O2生成效率由于其重原子效应而在pH值下活化。包封后,纳米探针可通过cRGD靶向富含αvβ3整联蛋白的肿瘤细胞,并被生理酸性pH激活以区分癌症和PDT。纳米探针的引人入胜的优势是800 nm以上的近红外实现,这显着提高了成像灵敏度并增加了PDT的穿透深度。通过监测PDT后肿瘤区域中荧光的减少,可以现场和实时地证明治疗效果,这为PDT功效跟踪提供了宝贵而方便的自我反馈功能。因此,这种经过合理设计和精心设计的纳米探针为精确的肿瘤治疗提供了新的范例,并可能为未来的临床癌症治疗提供新的机会。

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