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用于氧化还原刺激触发释放的新型双靶向线粒体和CD44受体纳米颗粒

Novel Dual Mitochondrial and CD44 Receptor Targeting Nanoparticles for Redox Stimuli-Triggered Release.

作者信息

Wang Kaili, Qi Mengjiao, Guo Chunjing, Yu Yueming, Wang Bingjie, Fang Lei, Liu Mengna, Wang Zhen, Fan Xinxin, Chen Daquan

机构信息

Collaborative Innovation Center of Advanced Drug Delivery System and Biotech Drugs in Universities of Shandong, School of Pharmacy, Yantai University, Yantai, China.

出版信息

Nanoscale Res Lett. 2018 Feb 2;13(1):32. doi: 10.1186/s11671-018-2445-1.

Abstract

In this work, novel mitochondrial and CD44 receptor dual-targeting redox-sensitive multifunctional nanoparticles (micelles) based on oligomeric hyaluronic acid (oHA) were proposed. The amphiphilic nanocarrier was prepared by (5-carboxypentyl)triphenylphosphonium bromide (TPP), oligomeric hyaluronic acid (oHA), disulfide bond, and curcumin (Cur), named as TPP-oHA-S-S-Cur. The TPP targeted the mitochondria, the antitumor drug Cur served as a hydrophobic core, the CD44 receptor targeting oHA worked as a hydrophilic shell, and the disulfide bond acted as a connecting arm. The chemical structure of TPP-oHA-S-S-Cur was characterized by HNMR technology. Cur was loaded into the TPP-oHA-S-S-Cur micelles by self-assembly. Some properties, including the preparation of micelles, morphology, redox sensitivity, and mitochondrial targeting, were studied. The results showed that TPP-oHA-S-S-Cur micelles had a mean diameter of 122.4 ± 23.4 nm, zeta potential - 26.55 ± 4.99 mV. In vitro release study and cellular uptake test showed that TPP-oHA-S-S-Cur micelles had redox sensibility, dual targeting to mitochondrial and CD44 receptor. This work provided a promising smart multifunctional nanocarrier platform to enhance the solubility, decrease the side effects, and improve the therapeutic efficacy of anticancer drugs.

摘要

在本研究中,我们提出了一种基于低聚透明质酸(oHA)的新型线粒体和CD44受体双靶向氧化还原敏感型多功能纳米颗粒(胶束)。两亲性纳米载体由(5-羧基戊基)三苯基溴化鏻(TPP)、低聚透明质酸(oHA)、二硫键和姜黄素(Cur)制备而成,命名为TPP-oHA-S-S-Cur。TPP靶向线粒体,抗肿瘤药物Cur作为疏水核心,靶向CD44受体的oHA作为亲水外壳,二硫键作为连接臂。通过HNMR技术对TPP-oHA-S-S-Cur的化学结构进行了表征。Cur通过自组装被载入TPP-oHA-S-S-Cur胶束中。研究了胶束的一些性质,包括胶束的制备、形态、氧化还原敏感性和线粒体靶向性。结果表明,TPP-oHA-S-S-Cur胶束的平均直径为122.4±23.4nm,zeta电位为-26.55±4.99mV。体外释放研究和细胞摄取试验表明,TPP-oHA-S-S-Cur胶束具有氧化还原敏感性,对线粒体和CD44受体具有双靶向性。这项工作提供了一个有前景的数据智能多功能纳米载体平台,以提高抗癌药物的溶解度,降低副作用,并提高治疗效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d425/5796929/603c7d33aae2/11671_2018_2445_Fig1_HTML.jpg

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