[12]aneN3-modified camptothecin and PEGylated AIEgens co-assembly into core–shell nanoparticles with ROS/NTR dual-response for enhanced cancer therapy†

IF 6.1 3区 医学 Q1 MATERIALS SCIENCE, BIOMATERIALS
Xue-Yi Sun, Ya-Xuan Liang, Yi-Nan Gao, Xi Zhang, Rui Liu, Quan Tang, Zhong-Lin Lu and Yang Liu
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引用次数: 0

Abstract

A novel dual-responsive nanoparticle (NP) system was aimed to be developed for the co-delivery of camptothecin (CPT) and plasmid encoding TNF-related apoptosis-inducing ligand (pTRAIL) DNA in cancer therapy. The combination of the prodrug CPT and the nucleic acid condensing di-(triazole-[12]aneN3) unit with 4-nitrobenzyl ester through alkyl chains resulted in three nitroreductase (NTR) responsive amphiphiles, CNN1–CNN3 (with 5, 8, and 11 carbon chains, respectively). Among them, CNN2 was the most effective in inhibiting the proliferation of HeLa cells in the presence of fusogenic lipid DOPE. The NPs composed of CNN2, pDNA, and DOPE were further co-assembled with ROS-responsive thioketal-linked amphiphilic polymer (TTP) to afford the core–shell NPs (CNN2-DT/pDNA) with an average size of 118 nm, which exhibited high drug-loading capacity, excellent serum tolerance, and good biocompatibility. In the presence of ROS, NTR, and NADH, the core–shell NPs were decomposed, leading to the efficient release of 80% CPT and abundant pDNA. The self-assembly and delivery process of CNN2-DT NPs and DNA were clearly observed through the AIE fluorescent imaging. In vitro and in vivo results demonstrated that the CNN2-DT/pTRAIL NPs synergistically promoted 68% apoptosis of tumor cells and inhibited tumor growth with negligible toxic side effects. This study showed that the combination of prodrug and nucleic acid through dual-responsive core–shell NPs provide a spatially and temporally-controlled strategy for cancer therapy.

Abstract Image

[12] ANN3-修饰的喜树碱和PEG化的AIEgens共组装成核壳纳米颗粒,具有ROS/NTR双重反应,用于增强癌症治疗†
开发了一种新型的双响应纳米粒子(NP)系统,用于在癌症治疗中同时递送喜树碱(CPT)和编码TNF-相关凋亡诱导配体(pTRAIL)DNA的质粒。前药CPT和核酸通过烷基链与4-硝基苄基酯缩合的二-(三唑-[12]aneN3)单元的组合产生了三种对硝基还原酶(NTR)有反应的两亲物CNN1–CNN3(分别具有5、8和11个碳链)。其中,在融合性脂质DOPE存在下,CNN2对HeLa细胞增殖的抑制作用最强。将由CNN2、pDNA和DOPE组成的NPs与ROS响应性硫酮连接的两亲性聚合物(TTP)进一步共组装,得到平均尺寸为118nm的核壳NPs(CNN2-DT/pDNA),其表现出高载药能力、优异的血清耐受性和良好的生物相容性。在ROS、NTR和NADH存在的情况下,核壳NP被分解,导致80%的CPT和丰富的pDNA的有效释放。通过AIE荧光成像,可以清楚地观察到CNN2-DT NPs和DNA的自组装和递送过程。体外和体内结果表明,CNN2-DT/pTRAIL NPs协同促进68%的肿瘤细胞凋亡并抑制肿瘤生长,毒副作用可忽略不计。这项研究表明,前药和核酸通过双反应核壳NP的组合为癌症治疗提供了一种空间和时间控制策略。
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来源期刊
Journal of Materials Chemistry B
Journal of Materials Chemistry B MATERIALS SCIENCE, BIOMATERIALS-
CiteScore
11.50
自引率
4.30%
发文量
866
期刊介绍: Journal of Materials Chemistry A, B & C cover high quality studies across all fields of materials chemistry. The journals focus on those theoretical or experimental studies that report new understanding, applications, properties and synthesis of materials. Journal of Materials Chemistry A, B & C are separated by the intended application of the material studied. Broadly, applications in energy and sustainability are of interest to Journal of Materials Chemistry A, applications in biology and medicine are of interest to Journal of Materials Chemistry B, and applications in optical, magnetic and electronic devices are of interest to Journal of Materials Chemistry C.Journal of Materials Chemistry B is a Transformative Journal and Plan S compliant. Example topic areas within the scope of Journal of Materials Chemistry B are listed below. This list is neither exhaustive nor exclusive: Antifouling coatings Biocompatible materials Bioelectronics Bioimaging Biomimetics Biomineralisation Bionics Biosensors Diagnostics Drug delivery Gene delivery Immunobiology Nanomedicine Regenerative medicine & Tissue engineering Scaffolds Soft robotics Stem cells Therapeutic devices
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