Curcumin-loaded Chitosan-Agarose-Montmorillonite Hydrogel Nanocomposite for the Treatment of Breast Cancer

A. Samadi, Shabnam Haseli, Mehrab Pourmadadi, H. Rashedi, F. Yazdian, M. Navaei-Nigjeh
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引用次数: 23

Abstract

Cancer has been one of the leading causes of death worldwide. Chemotherapy is a proposed therapeutic in recent years; however, its efficiency is restricted due to multiple drug resistance (MDR), toxicity on normal cells, and poor physicochemical properties. The use of natural compounds with less cytotoxicity on normal cells is a promising approach to cancer treatment. Curcumin (CUR) is a plant flavonol from the flavonoid group of polyphenols with anti-tumor activity. Nonetheless, low solubility, poor permeability, and short biological half-life hamper the use of curcumin as an anti-cancer drug. The principal aim of this study was to augment CUR loading as a hydrophobic drug and prolong the release time. Curcumin was loaded into a hydrogel nanocomposite of chitosan (CS)-agarose (AG)-montmorillonite (MMT) to attain this goal. The use of MMT nanoparticles in the CS-AG hydrogel improved the loading efficiency from 49% to 62%. The average diameter of the nanocomposite particles in the FESEM images was within the range of 30 nm. Zeta potential of the hydrogel nanocomposites was 47mV, which demonstrates the good stability of the hydrogel nanocomposites. The inclusion of all components in the nanocomposite was proved through the presence of all of the characteristic peaks of the components in the FTIR spectrum. The drug release profile showed the pH-responsive behavior of CS-AG-MMT hydrogel nanocomposites with extended-release over 96 h. The cytotoxicity of fabricated nanocomposites on the MCF-7 cell line was evaluated. Curcumin-loaded CS-AG-MMT showed significant cytotoxicity compared to the control group (p<0.001) and curcumin as a free drug (p<0.05). The developed nanostructure is a promising vehicle with the potential to enhance curcumin loading and achieve sustained release of curcumin with significant cytotoxicity on MCF-7 cells.
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载姜黄素壳聚糖-琼脂糖-蒙脱土水凝胶纳米复合材料治疗乳腺癌
癌症一直是世界范围内导致死亡的主要原因之一。化疗是近年来提出的一种治疗方法;然而,由于耐多药、对正常细胞有毒性、理化性质差等原因,其效率受到限制。在正常细胞上使用具有较少细胞毒性的天然化合物是一种很有前途的癌症治疗方法。姜黄素(Curcumin, CUR)是一类具有抗肿瘤活性的植物多酚类黄酮醇。然而,溶解度低、渗透性差、生物半衰期短阻碍了姜黄素作为抗癌药物的应用。本研究的主要目的是增加CUR作为疏水药物的负载并延长释放时间。将姜黄素装入壳聚糖(CS)-琼脂糖(AG)-蒙脱土(MMT)的水凝胶纳米复合材料中以达到这一目的。在CS-AG水凝胶中使用MMT纳米颗粒将负载效率从49%提高到62%。在FESEM图像中,纳米复合颗粒的平均直径在30 nm范围内。水凝胶纳米复合材料的Zeta电位为47mV,表明水凝胶纳米复合材料具有良好的稳定性。通过FTIR光谱中所有组分的特征峰的存在,证明了纳米复合材料中包含了所有组分。药物释放谱显示CS-AG-MMT水凝胶纳米复合材料具有ph响应行为,缓释时间超过96 h。含有姜黄素的CS-AG-MMT与对照组相比具有显著的细胞毒性(p<0.001),与姜黄素作为游离药物相比(p<0.05)。所开发的纳米结构是一种很有前途的载体,具有增强姜黄素负载和实现姜黄素持续释放的潜力,对MCF-7细胞具有显著的细胞毒性。
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