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首页> 外文期刊>Acta biomaterialia >Boronic acid-tethered amphiphilic hyaluronic acid derivative-based nanoassemblies for tumor targeting and penetration
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Boronic acid-tethered amphiphilic hyaluronic acid derivative-based nanoassemblies for tumor targeting and penetration

机译:硼酸拴系的两亲透明质酸衍生物的肿瘤靶向瘤靶向和渗透

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摘要

(3-Aminomethylphenyl)boronic acid (AMPB)-installed hyaluronic acid-ceramide (HACE)-based nanopartides (NPs), including manassantin B (MB), were fabricated for tumor-targeted delivery. The amine group of AMPS was conjugated to the carboxylic acid group of hyaluronic acid (HA) via amide bond formation, and synthesis was confirmed by spectroscopic methods. HACE-AMPB/MB NPs with a 239-nm mean diameter, narrow size distribution, negative zeta potential, and >90% drug encapsulation efficiency were fabricated. Exposed AMPB in the outer surface of HACE-AMPB NPs (in the aqueous environment) may react with sialic acid of cancer cells. The improved cellular accumulation efficiency, in vitro antitumor efficacy, and tumor penetration efficiency of HACE-AMPB/MB NPs, compared with HACE/MB NPs, in MDA-MB-231 cells (CD44 receptor-positive human breast adenocarcinoma cells) may be based on the CD44 receptor mediated endocytosis and phenylboronic acid-sialic acid interaction. Enhanced in vivo tumor targetability, infiltration efficiency, and antitumor efficacies of HACE-AMPB NPs, compared with HACE NPs, were observed in a MDA-MB-231 tumor-xenografted mouse model. In addition to passive tumor targeting (based on an enhanced permeability and retention effect) and active tumor targeting (interaction between HA and CD44 receptor), the phenylboronic acid-sialic acid interaction can play important roles in augmented tumor targeting and penetration of HACE-AMPB NPs.
机译:(3-氨基甲基苯基)硼酸(AMPB) - 组合的透明质酸 - 神经酰胺(HACE)基于纳米丙醇(NPS),包括Manandantin B(MB),用于肿瘤靶向递送。通过酰胺键形成将胺基AMPS与透明质酸(HA)的羧酸基团缀合,并通过光谱方法证实合成。 HACE-AMPB / MB NPS具有239mm平均直径,窄尺寸分布,负ZETA电位和> 90%的药物包封效率。 Hace-Ampb nps(在水环境中)外表面的暴露的ampb可以与癌细胞的唾液酸反应。与Hace-Ampb / MB NPS的细胞累积效率,体外抗肿瘤功效和肿瘤渗透效率,与HECE / MB NPS相比,在MDA-MB-231细胞中(CD44受体阳性人乳腺腺癌细胞)可以是基于的CD44受体介导的内吞作用和苯硼酸 - 唾液酸相互作用。在MDA-MB-231肿瘤 - 异种移植小鼠模型中观察到与HCE-AMPB NPS相比,HACE-AMPB NP的肿瘤靶向,渗透效率和抗肿瘤疗效增强。除了被动肿瘤靶向(基于增强的渗透率和保留效果)和活性肿瘤靶向(HA和CD44受体之间的相互作用),苯基硼酸 - 唾液酸相互作用可以在增强肿瘤靶向和HACE-AMPB的渗透中起重要作用nps。

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