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胆固醇和维生素 E 修饰的聚乙二醇化聚合物胶束用于姜黄素的高效传递和增强抗癌活性:在 2D 单层和 3D 球体中的评估。

Cholesterol and vitamin E-conjugated PEGylated polymeric micelles for efficient delivery and enhanced anticancer activity of curcumin: evaluation in 2D monolayers and 3D spheroids.

机构信息

a Department of Pharmacy , Birla Institute of Technology & Science-Pilani, Hyderabad Campus , Hyderabad , India.

出版信息

Artif Cells Nanomed Biotechnol. 2018;46(sup1):773-786. doi: 10.1080/21691401.2018.1435551. Epub 2018 Feb 9.

DOI:10.1080/21691401.2018.1435551
PMID:29426248
Abstract

A newly synthesized PEGylated cholesterol/α-tocopheryl succinate (α-TOS) linked polymer (CV) was self-assembled and loaded with curcumin to form a micellar system (C-CVM). The tri-functionalized amphiphilic polymer was constituted of hydrophobic cholesterol and α-TOS connected to hydrophilic PEG via a lysine linker. The synthesized polymer and the micelles were characterized by H NMR, DLS, zeta potentiometer, TEM, CMC determination and hemolysis studies. CVM displayed low CMC value of 15 µM with extent of hemolysis as less than 4%. The stable C-CVM with optimum % drug loading (14.2 ± 0.24) displayed Z average of 175.8 ± 0.68 nm with PDI (0.248 ± 0.075) and released curcumin in sustained manner in the in vitro drug release study. C-CVM demonstrated dose-dependent cellular uptake and cytotoxicity in murine melanoma, B16F10 and human breast cancer, MDA-MB-231 cell lines. CV exhibited marked reversal of drug resistance as indicated by significantly higher retention of P-glycoprotein substrate, rhodamine-123 in the resistant B16F10 cell line compared to standard P-glycoprotein inhibitor, verapamil. C-CVM demonstrated significantly higher spheroidal growth inhibition compared to C-PPM. The results provide strong evidence for CVM as promising drug delivery system and confirm the potential of C-CVM as chemotherapy in cancer.

摘要

一种新合成的聚乙二醇化胆固醇/生育酚琥珀酸酯(α-TOS)连接聚合物(CV)自组装并负载姜黄素形成胶束系统(C-CVM)。三功能两亲聚合物由疏水胆固醇和α-TOS 通过赖氨酸接头连接到亲水 PEG 组成。合成聚合物和胶束通过 H NMR、DLS、zeta 电位计、TEM、CMC 测定和溶血研究进行了表征。CVM 显示出低 CMC 值为 15µM,溶血程度小于 4%。具有最佳载药量(14.2±0.24%)的稳定 C-CVM 显示 Z 平均为 175.8±0.68nm,PDI(0.248±0.075),并在体外药物释放研究中以持续方式释放姜黄素。C-CVM 在小鼠黑色素瘤、B16F10 和人乳腺癌 MDA-MB-231 细胞系中表现出剂量依赖性细胞摄取和细胞毒性。CV 表现出明显的逆转耐药性,因为与标准 P-糖蛋白抑制剂维拉帕米相比,耐药 B16F10 细胞系中罗丹明 123 的保留率显著更高。C-CVM 显示出比 C-PPM 更高的球形生长抑制率。这些结果为 CVM 作为有前途的药物递送系统提供了有力证据,并证实了 C-CVM 作为癌症化疗的潜力。

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引用本文的文献

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