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酶指导的自组装形成的超分子纳米纤维用于 SKBR-3 细胞选择性抑制。

Supramolecular Nanofibers Formed by Enzyme-Instructed Self-Assembly for SKBR-3 Cell Selective Inhibition.

机构信息

Department of Radiotherapy, Shandong Cancer Hospital and Institute, Shandong First Medical University and Shandong Academy of Medical Sciences, 250117, Jinan, P. R. China.

Cheeloo College of Medicine, Shandong University, 250100, Jinan, P. R. China.

出版信息

Chem Asian J. 2022 Jul 15;17(14):e202200301. doi: 10.1002/asia.202200301. Epub 2022 May 23.

Abstract

Cell-targeted peptides are recommended for precision cancer treatment due to their comparable targeting properties, small molecular size, and good biocompatibility. However, unpredictable bioactivity, low penetration rate and poor stability greatly limit its efficacy. Supramolecular self-assembly based on synthetic peptide has great potential to solve related problems and achieve better therapeutic effects. Herein, we report and compare the effects of two different assembly pathway, heating-cooling, and enzyme instruction, on the penetrability of SKBR-3 cell targeted peptides. It was found that enzyme-instructed self-assembly (EISA) resulted in hydrogels composed of uniform supramolecular nanofibers, whereas heating-cooling resulted in solutions and precipitations composed of slightly different nanoparticles. The nanofibers formed by EISA showed enhanced cellular uptake (2.54 μM), which was significantly higher than the 1.06 μM of the nanoparticles formed by temperature regulation. Thus, EISA is a promising strategy to improve the cell penetration rate of targeted peptides and could provide a better solution for precision cancer treatment.

摘要

细胞靶向肽由于其靶向性能相当、分子尺寸小、良好的生物相容性,被推荐用于精准癌症治疗。然而,不可预测的生物活性、低穿透率和较差的稳定性极大地限制了其疗效。基于合成肽的超分子自组装具有很大的潜力来解决相关问题并实现更好的治疗效果。在此,我们报告并比较了两种不同的组装途径,即加热-冷却和酶指令,对 SKBR-3 细胞靶向肽穿透性的影响。结果发现,酶指令自组装(EISA)导致由均匀的超分子纳米纤维组成的水凝胶,而加热-冷却导致由略微不同的纳米颗粒组成的溶液和沉淀。EISA 形成的纳米纤维表现出增强的细胞摄取(2.54 μM),明显高于由温度调节形成的纳米颗粒的 1.06 μM。因此,EISA 是一种提高靶向肽细胞穿透率的有前途的策略,可为精准癌症治疗提供更好的解决方案。

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