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一种近红外激光触发的尺寸可收缩纳米系统,具有原位药物释放功能,可实现深层肿瘤穿透。

A Near-Infrared Laser-Triggered Size-Shrinkable Nanosystem with In Situ Drug Release for Deep Tumor Penetration.

机构信息

College of Pharmaceutical Sciences, Zhejiang University of Technology, Hangzhou 310014, P.R. China.

出版信息

ACS Appl Mater Interfaces. 2021 Apr 14;13(14):16036-16047. doi: 10.1021/acsami.1c00022. Epub 2021 Mar 18.

Abstract

The development of smart size-tunable drug delivery nanoplatform enables the solving of the paradox of inconsistent size-dependence of high tumor accumulation and deep penetration during its delivery process, thus achieving superior cancer treatment efficacy. Herein, we report a size-shrinkable nanomicelle complex system with an initial size of 101 nm enabling effective retention around the tumor periphery and could destruct to ultrasmall nanomicelles triggered by a near-infrared (NIR) laser to realize the deep tumor penetration. The nanomicelle system is consisted of an upper critical solution temperature (UCST)-type block copolymer poly(acrylamide-acrylonitrile)-polyethylene glycol-lipoic acid (p(AAm--AN)--PEG-LA) encapsulating gold nanorods. Upon the irradiation of the NIR laser at the tumor site, gold nanorods could convert the light energy to heat energy, realizing the photothermal ablation of superficial tumor tissue. Concurrently, the large micelles split into a cascade of ultrasmall micelles (∼7 nm), which could easily penetrate into the deep site of the tumor and achieve the in situ "on-demand" release of the loaded drug to exert superior combined photothermal-chemotherapy of cancer. By the precise manipulation of laser, the micelle complex system realized the hierarchical killing from the superficial-to-deep tumor and achieved almost complete tumor growth inhibition on the established xenograft liver tumor mice model.

摘要

智能尺寸可调药物递送纳米平台的发展使解决药物递送过程中高肿瘤积累与深穿透之间的尺寸依赖性矛盾成为可能,从而实现了卓越的癌症治疗效果。在此,我们报告了一种尺寸可缩小的纳米胶束复合体系,其初始尺寸为 101nm,能够有效地保留在肿瘤周围,并能够在近红外(NIR)激光的触发下分解为超小纳米胶束,从而实现深肿瘤穿透。该纳米胶束体系由上临界溶解温度(UCST)型嵌段共聚物聚(丙烯酰胺-丙烯腈)-聚乙二醇-脂酸(p(AAm--AN)-PEG-LA)包封金纳米棒组成。在肿瘤部位照射近红外激光时,金纳米棒可以将光能转化为热能,实现浅表肿瘤组织的光热消融。同时,大胶束分裂成一连串的超小胶束(~7nm),可以轻易穿透肿瘤深部,并实现原位“按需”释放负载药物,从而发挥出色的光热化疗联合治疗癌症的效果。通过激光的精确操作,胶束复合体系实现了从浅表到深部肿瘤的分级杀伤,在建立的异种移植肝肿瘤小鼠模型上几乎完全抑制了肿瘤生长。

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