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ICG 赋能的可变形纳米治疗剂:在近红外光照射下增强肿瘤穿透性。

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

机构信息

Department of Nanomedicine and Biopharmaceuticals, College of Life Science and Technology, Huazhong University of Science and Technology, Wuhan, 430074, China.

出版信息

Nanoscale. 2019 Mar 28;11(13):6217-6227. doi: 10.1039/c9nr01049a.

Abstract

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.

摘要

肿瘤渗透是当前癌症纳米医学的瓶颈,限制了其在临床上的最终抗肿瘤疗效。在此,我们利用众所周知的吲哚菁绿(ICG)的不稳定性,报告了近红外(NIR)光响应纳米颗粒(NP)的制备,以增强肿瘤渗透。ICG 通过非共价相互作用交联羟乙基淀粉(HES)和阿霉素(DOX)缀合物(HES-SS-DOX),促进 ICG@HES-SS-DOX NP 的形成。ICG 的光触发降解导致这种 NP 的解离,并且由于 ICG 的光热效应,所得到的 HES-SS-DOX 已被证明在 H22 肿瘤球体和荷瘤小鼠中渗透更深。因此,可分解的 ICG@HES-SS-DOX NP 比其原本在 NIR 光刺激下无法解离的对应物具有更好的肿瘤穿透能力。所报道的 ICG@HES-SS-DOX NP 可能对治疗具有密集细胞外基质的恶性肿瘤(如肝癌和胰腺癌)具有强大的疗效。这项研究为癌症纳米治疗学开辟了一种新的 FDA 批准的 ICG 功能。

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