使用双配体安装的靶向药物递送系统向癌细胞和线粒体内递送药物

IF 5.5 2区 材料科学 Q2 MATERIALS SCIENCE, MULTIDISCIPLINARY
Purvi Kishore, , , Sourav Barman, , , Rimpa Dey, , , Ankita Jana, , , Malabika Ghosh, , , Pousali Bag, , , Tapas Ghatak, , , Partha Sona Maji, , , Chitrita Ghosh, , , Nayana Mukherjee, , , Ankan Dutta Chowdhury, , , Souvik Ghatak, , , Rupam Mukherjee, , , Arnab Basu, , , Ali Hossain Khan, , , Surya K. Ghosh, , , Sadananda Mandal, , and , Amit Ranjan Maity*, 
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引用次数: 0

摘要

由于药物的脱靶毒性,传统的抗癌治疗面临很大的局限性。一种专门的药物输送系统(DDS)已被证明是克服这一障碍的潜在方法。靶向给药不仅提高了药物定位的精度,而且通过进一步将治疗药物选择性地引导到特定细胞内细胞器内的作用部位,将药物的不良反应降至最低。在各种靶点中,叶酸受体在许多癌症类型中表现出显着较高的表达水平,使其适合临床前开发。此外,在将抗癌药物选择性地递送到癌细胞后,细胞内运输过程的调节也可能影响药物作用的效果。通过在同一DDS表面上使用两种不同类型的靶向配体,可以实现对癌细胞的选择性靶向和将药物递送到其作用位点。在本研究中,我们使用了一种壳聚糖为基础的生物聚合物,通过简单的化学方法对胆固醇分子进行修饰,并安装了双配体,叶酸(FA)和三苯基膦(TPP),用于选择性靶向癌细胞和进一步的姜黄素线粒体递送。在过表达叶酸受体的KB细胞中进行细胞摄取研究,利用荧光显微镜和流式细胞术分析证实,靶向DDS的细胞摄取分别比非靶向DDS(没有TPP修饰)和空DDS(表面没有FA和TPP)高许多倍,对癌细胞产生更大的细胞毒性作用。所开发的用于聚合物合成和配体修饰的化学方法是一个简单、直接和一步的过程,它产生了一个多功能和多方面的DDS,可以封装各种各样的药物(疏水、带电、小分子、生物分子药物等)和配体,以增强精确治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Delivering Drugs to Cancer Cells and inside the Mitochondria Using a Dual-Ligand Installed Targeted Drug Delivery System

Delivering Drugs to Cancer Cells and inside the Mitochondria Using a Dual-Ligand Installed Targeted Drug Delivery System

Traditional anticancer therapy faces major limitations due to the off-target toxicity of drugs. A specialized drug delivery system (DDS) has proven to be a potential approach for overcoming this barrier. Targeted delivery to cancer cells not only enhances the precision of drug localization but also minimizes adverse effects of the drug by further directing therapeutic agents selectively to their site of action inside specific intracellular organelles. Among various targets, folate receptors show a significantly higher level of expression in many cancer types, making them suitable for preclinical developments. Moreover, after this selective delivery of anticancer drugs to cancer cells, regulation of the intracellular trafficking process could also impact the efficacy of drug actions. This selective targeting of cancer cells and delivery of drugs to their sites of action could be achieved by using two different types of targeting ligands on the same DDS surface. Herein, we used a chitosan-based biopolymer, modified by cholesterol molecules using a simple chemical approach and installed dual ligands, folic acid (FA) and triphenylphosphine (TPP) for selective cancer cell targeting and further mitochondrial delivery of curcumin. Cellular uptake studies in KB cells, which overexpress folate receptors, using fluorescence microscopy and flow cytometry analysis confirmed that the targeted DDS has many-fold higher cellular uptake than the nontargeted DDS (without decoration of TPP) and the null DDS (without FA and TPP on its surface), respectively, which induced more cytotoxic effects on cancer cells. The developed chemical approach employed for polymer synthesis and ligand decoration is a simple, straightforward, and one-step process that generates a versatile and multifaceted DDS with the possibility to encapsulate a wide variety of drugs (hydrophobic, charged, small molecule, biomolecule drugs, etc.) and ligands for enhanced precision therapy.

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来源期刊
CiteScore
8.30
自引率
3.40%
发文量
1601
期刊介绍: ACS Applied Nano Materials is an interdisciplinary journal publishing original research covering all aspects of engineering, chemistry, physics and biology relevant to applications of nanomaterials. The journal is devoted to reports of new and original experimental and theoretical research of an applied nature that integrate knowledge in the areas of materials, engineering, physics, bioscience, and chemistry into important applications of nanomaterials.
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