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聚(光敏剂)纳米粒子通过中断 π-π 堆积和延长循环时间来增强体内光动力治疗。

Poly(photosensitizer) Nanoparticles for Enhanced in Vivo Photodynamic Therapy by Interrupting the π-π Stacking and Extending Circulation Time.

机构信息

State Key Laboratory of Fine Chemicals, School of Chemical Engineering , Dalian University of Technology , Linggong Rd. 2 , Dalian , Liaoning 116023 , China.

Department of Comparative Medicine Laboratory Animal Center , Dalian Medical University , No. 9 Lvshun South Road , Dalian , Liaoning 116000 , China.

出版信息

ACS Appl Mater Interfaces. 2019 May 22;11(20):18224-18232. doi: 10.1021/acsami.9b04351. Epub 2019 May 13.

Abstract

The natural planar and rigid structures of most of the hydrophobic photosensitizers (PSs) [such as tetraphenyl porphyrin (TPP)] significantly reduce their loading efficiencies in polymeric nanoparticles (NPs) because of the strong π-π interaction-induced aggregation. This aggregation-caused quenching will further reduce the quantum yield of singlet oxygen (O) generation and weaken the efficiency of photodynamic therapy (PDT). In addition, the small molecular PSs exhibit short tumor retention time and tend to be easily cleared once released. Herein, poly(TPP) NPs, prepared by cross-linking of reactive oxygen species degradable, thioketal linkers and TPP derivatives, followed by coprecipitation, were first developed with quantitative loading efficiency (>99%), uniform NP sizes (without aggregation), increased singlet oxygen quantum yield (Φ = 0.79 in dimethyl sulfoxide compared with 0.52 for original TPP), increased in vitro phototoxicity, extended tumor retention time, light-triggered on-demand release, and enhanced in vivo antitumor efficacy, which comprehensively address the multiple issues for most of the PSs in the PDT area.

摘要

大多数疏水性光敏剂(PSs)[如四苯基卟啉(TPP)]的天然平面和刚性结构,由于强π-π相互作用诱导的聚集,大大降低了它们在聚合物纳米颗粒(NPs)中的负载效率。这种聚集引起的猝灭将进一步降低单线态氧(O)生成的量子产率,并削弱光动力疗法(PDT)的效率。此外,小分子 PSs 表现出短的肿瘤保留时间,并且一旦释放,往往容易被清除。在此,通过交联具有反应性氧物种降解、硫缩酮键和 TPP 衍生物的聚(TPP)纳米颗粒,首先以定量的负载效率(>99%)、均匀的 NP 尺寸(无聚集)、增加的单线态氧量子产率(在二甲基亚砜中为 0.79,而原始 TPP 为 0.52)、体外光毒性增加、延长肿瘤保留时间、光触发按需释放和增强体内抗肿瘤功效,综合解决了 PDT 领域中大多数 PSs 的多个问题。

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