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Transformable nanotherapeutics enabled by ICG: towards enhanced tumor penetration under NIR light irradiation

机译:可变形的纳米疗法通过协调小组:对增强肿瘤渗透在近红外光谱光照射

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摘要

Tumor penetration is the bottleneck for current cancer nanomedicine, limiting the ultimate antitumor efficacy in the clinic. Herein, by exploiting the well-known instability of indocyanine green (ICG), we report the preparation of near infrared (NIR) light responsive nanoparticles (NP) for enhanced tumor penetration. ICG crosslinks hydroxyethyl starch (HES) and doxorubicin (DOX) conjugates (HES-SS-DOX) via noncovalent interactions, facilitating the formation of ICG@HES-SS-DOX NP. The light triggered degradation of ICG leads to the dissociation of such NP, and the resulting HES-SS-DOX has been shown to penetrate deeper in both H22 tumor spheroids and tumor bearing mice, due to the photothermal effect of ICG. Therefore, the disintegrable ICG@HES-SS-DOX NP have better tumor penetration capacity than their counterparts, which originally cannot dissociate under NIR light stimulation. The reported ICG@HES-SS-DOX NP might be potent in treating malignant tumors with dense extracellular matrices, such as liver and pancreatic cancers. This study opens up a novel functionality of FDA-approved ICG for cancer nanotherapeutics.
机译:肿瘤是当前的瓶颈渗透癌症纳米,限制的终极在临床抗肿瘤功效。利用著名的不稳定吲哚菁绿(ICG)我们报告制备近红外(NIR)光响应性纳米粒子(NP)增强肿瘤渗透。(他)和阿霉素(阿霉素)配合(HES-SS-DOX)通过共价相互作用,促进ICG@HES-SS-DOX NP的形成。协调小组导致的光触发退化此类NP的离解和由此产生的HES-SS-DOX可以穿透更深两种小鼠H22肿瘤和肿瘤球状体轴承,由于协调小组的光照效果。的disintegrable ICG@HES-SS-DOX NP有更好的肿瘤穿透能力比他们同行,原本不能分离在近红外光谱光刺激。ICG@HES-SS-DOX NP可能有效的治疗恶性肿瘤与细胞外矩阵,如肝脏和胰腺癌症。本研究打开了一个小说的功能fda批准为癌症纳米疗法协调小组。

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