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两亲性接枝共聚物琥珀酸-α-生育酚-γ-羧甲基壳聚糖在调节他莫昔芬的渗透性和抗癌疗效方面的潜力。

Potential of amphiphilic graft copolymer α-tocopherol succinate-g-carboxymethyl chitosan in modulating the permeability and anticancer efficacy of tamoxifen.

作者信息

Jena Sunil K, Samal Sanjaya K, Kaur Shamandeep, Chand Mahesh, Sangamwar Abhay T

机构信息

Department of Pharmaceutical Technology (Formulations), National Institute of Pharmaceutical Education and Research, Sector-67, S.A.S. Nagar, Punjab 160062, India.

Department of Pharmaceutics, National Institute of Pharmaceutical Education and Research, Sector-67, S.A.S. Nagar, Punjab 160062, India.

出版信息

Eur J Pharm Sci. 2017 Apr 1;101:149-159. doi: 10.1016/j.ejps.2017.02.023. Epub 2017 Feb 16.

DOI:10.1016/j.ejps.2017.02.023
PMID:28214545
Abstract

Recent studies showed an enhanced oral bioavailability of tamoxifen (TMX) by hydrophobically modified α-tocopherol succinate-g-carboxymethyl chitosan (Cmc-TS) micelles. As a continued effort, here we evaluated TMX-loaded polymeric micelles (TMX-PMs) for its enhanced permeability with increased anticancer efficacy and decreased hepatotoxicity. We employed co-solvent evaporation technique to encapsulate TMX into Cmc-TS. Apparent permeability assay of TMX-PMs was performed on Caco-2 cell line. The absorptive transport of TMX increased significantly about 3.8-fold when incorporated into Cmc-TS PMs. Cytotoxicity of Cmc-TS PMs was studied on MCF-7 cell line by MTT and; confocal microscopy was used for cellular uptake. Confocal microscopy revealed that Cmc-TS PMs could effectively accumulate in the cytosol of MCF-7 cell lines. In vitro data was further validated using N-methyl-N-nitrosourea (MNU)-induced mammary carcinogenesis model in Sprague-Dawley rats. Hepatotoxicity profiles of TMX-PMs at three different doses were also evaluated against the free drug TMX. TMX-PMs were more effective in suppressing breast tumor in MNU-induced mammary carcinoma model than free TMX with better safety profile. In addition, histological data shows that tumors are "benign" in TMX-PMs treated group compared with "malignant" tumors in free TMX treated and control groups. Overall, the results implicate that our Cmc-TS PMs may serve as a promising carrier for the intracellular delivery of anticancer drug molecules via oral route.

摘要

近期研究表明,疏水修饰的琥珀酸α-生育酚 -γ-羧甲基壳聚糖(Cmc-TS)胶束可提高他莫昔芬(TMX)的口服生物利用度。作为持续的研究工作,在此我们评估了载有TMX的聚合物胶束(TMX-PMs),其具有增强的渗透性,抗癌疗效增加且肝毒性降低。我们采用共溶剂蒸发技术将TMX封装到Cmc-TS中。在Caco-2细胞系上进行了TMX-PMs的表观渗透率测定。当TMX被包载到Cmc-TS胶束中时,其吸收转运显著增加了约3.8倍。通过MTT法在MCF-7细胞系上研究了Cmc-TS胶束的细胞毒性;共聚焦显微镜用于细胞摄取研究。共聚焦显微镜显示Cmc-TS胶束可有效积聚在MCF-7细胞系的细胞质中。使用N-甲基-N-亚硝基脲(MNU)诱导的Sprague-Dawley大鼠乳腺癌发生模型进一步验证了体外数据。还针对游离药物TMX评估了三种不同剂量的TMX-PMs的肝毒性情况。在MNU诱导的乳腺癌模型中,TMX-PMs在抑制乳腺肿瘤方面比游离TMX更有效,且安全性更好。此外,组织学数据表明,与游离TMX治疗组和对照组中的“恶性”肿瘤相比,TMX-PMs治疗组中的肿瘤为“良性”。总体而言,结果表明我们的Cmc-TS胶束可能作为一种有前景的载体,通过口服途径实现抗癌药物分子的细胞内递送。

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