Dual-targeted and viscosity-sensitive infrared AIE photosensitizer based on tumor microenvironmental response for photodynamic cancer therapy†

IF 2.7 3区 化学 Q2 CHEMISTRY, MULTIDISCIPLINARY New Journal of Chemistry Pub Date : 2024-11-04 DOI:10.1039/D4NJ03321C
Xiaoye Wen, Zhilin Shi, Yongfei Huang and Zhefeng Fan
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Abstract

Due to their excellent capabilities in photodynamic therapy (PDT) and aggregation-induced emission, (AIE) photosensitizers have attracted a great deal of attention. However, the poor water solubilities of current AIE photosensitizers limit their widespread in vivo application and PDT productivity. AIE photosensitizers with triphenylamine as electron-donating moiety and pyridine as electron-absorbing group can enhance the D–A effort, thus improving the intramolecular charge transfer (ICT) and extending the emission wavelength. At the same time, ΔEst was reduced and intersystem crossing processes was promoted due to the D–A effect of the photosensitizers, thus increasing the probability of ROS generation. Herein, a dual-organelle targeted and viscosity-sensitive infrared AIE photosensitizer (NES-OH) with a D–A structure was developed and synthesized. The NES-OH had good water solubility and good linear relationship with concentration. The NES-OH exhibited bright fluorescence at 620 nm with a quantum yield of 66.75% and had high 1O2 generation efficiency, as well as good biocompatibility and photostability. The NES-OH can target mitochondria and lysosomes and also monitor lysosomes and mitochondrial viscosity changes in real time or in situ in living cells. More interestingly, in the acidic environment of cancer cells, the structure of the NES-OH changed with the appearance of specific morpholine groups, leading to the targeting of lysosomes and further distinguishing and detecting normal and cancer cells. The in vitro and in vivo study demonstrated that the NES-OH can inhibit tumor growth efficiently upon light exposure. This work constructed an effective photosensitizer for diagnosing and treating cancers and evaluating PDT efficacy.

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基于肿瘤微环境响应的双靶向粘度敏感型红外 AIE 光敏剂用于癌症光动力疗法†。
由于光敏剂在光动力疗法(PDT)和聚集诱导发射(AIE)方面具有出色的能力,因此吸引了大量关注。然而,目前 AIE 光敏剂的水溶性较差,限制了它们在体内的广泛应用和光动力疗法的生产率。以三苯胺为给电子基团、吡啶为吸电子基团的 AIE 光敏剂可增强 D-A 作用,从而改善分子内电荷转移(ICT)并延长发射波长。同时,由于光敏剂的 D-A 效应,ΔEst 减少,系统间交叉过程得到促进,从而增加了 ROS 生成的概率。在此,我们开发并合成了一种具有D-A结构的双细胞器靶向粘度敏感型红外AIE光敏剂(NES-OH)。NES-OH 具有良好的水溶性,且与浓度呈良好的线性关系。NES-OH 在 620 纳米波长处发出明亮的荧光,量子产率高达 66.75%,具有很高的 1O2 生成效率,以及良好的生物相容性和光稳定性。NES-OH 可以靶向线粒体和溶酶体,还能实时或原位监测活细胞中溶酶体和线粒体的粘度变化。更有趣的是,在癌细胞的酸性环境中,NES-OH 的结构会发生变化,出现特定的吗啉基团,从而靶向溶酶体,进一步区分和检测正常细胞和癌细胞。体外和体内研究表明,NES-OH 在光照下可有效抑制肿瘤生长。这项工作构建了一种有效的光敏剂,可用于诊断和治疗癌症以及评估光动力疗法的疗效。
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来源期刊
New Journal of Chemistry
New Journal of Chemistry 化学-化学综合
CiteScore
5.30
自引率
6.10%
发文量
1832
审稿时长
2 months
期刊介绍: A journal for new directions in chemistry
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