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新型可生物降解且自组装的甲氧基聚(乙二醇)-棕榈酸酯纳米载体的合成,用于将姜黄素递送至癌细胞。

Synthesis of novel biodegradable and self-assembling methoxy poly(ethylene glycol)-palmitate nanocarrier for curcumin delivery to cancer cells.

作者信息

Sahu Abhishek, Bora Utpal, Kasoju Naresh, Goswami Pranab

机构信息

Biomaterials and Tissue Engineering Laboratory, Department of Biotechnology, Indian Institute of Technology Guwahati, Guwahati 781 039, Assam, India.

出版信息

Acta Biomater. 2008 Nov;4(6):1752-61. doi: 10.1016/j.actbio.2008.04.021. Epub 2008 May 11.


DOI:10.1016/j.actbio.2008.04.021
PMID:18524701
Abstract

A novel polymeric amphiphile, mPEG-PA, was synthesized with methoxy poly(ethylene glycol) (mPEG) as the hydrophilic and palmitic acid (PA) as the hydrophobic segment. The conjugate prepared in a single-step reaction showed minimal toxicity on HeLa cells. (1)H nuclear magnetic resonance imaging and Fourier transform infrared spectroscopy revealed that the conjugation was through an ester linkage, which is biodegradable. Enzymes having esterase activity, such as lipase, can degrade the conjugate easily, as observed by in vitro studies. mPEG-PA conjugate undergoes self-assembly in an aqueous environment, as evidenced by fluorescence spectroscopic studies with pyrene as a probe. The mPEG-PA conjugate formed micelles in the aqueous solution with critical micelle concentration of 0.12 g l(-1). Atomic force microscopy and dynamic light scattering studies showed that the micelles were spherical in shape, with a mean diameter of 41.43 nm. The utility of mPEG-PA to entrap the potent chemopreventive agent curcumin in the core of nanocarrier was investigated. The encapsulation of a highly hydrophobic compound like curcumin in the nanocarrier makes the drug readily soluble in an aqueous system, which can increase the ease of dosing and makes intravenous dosing possible. Drug-loaded micelle nanoparticles showed good stability in physiological condition (pH 7.4), in simulated gastric fluid (pH 1.2) and in simulated intestinal fluid (pH 6.8). This micellar formulation can be used as an enzyme-triggered drug release carrier, as suggested by in vitro enzyme-catalyzed drug release using pure lipase and HeLa cell lysate. The IC(50) of free curcumin and encapsulated curcumin was found to be 14.32 and 15.58 microM, respectively.

摘要

一种新型聚合物两亲物mPEG - PA,以甲氧基聚(乙二醇)(mPEG)作为亲水链段,棕榈酸(PA)作为疏水链段合成。在一步反应中制备的缀合物对HeLa细胞显示出最小的毒性。核磁共振成像和傅里叶变换红外光谱表明缀合物是通过可生物降解的酯键连接。如体外研究所示,具有酯酶活性的酶,如脂肪酶,可以很容易地降解缀合物。以芘为探针的荧光光谱研究证明,mPEG - PA缀合物在水环境中会发生自组装。mPEG - PA缀合物在水溶液中形成胶束,临界胶束浓度为0.12 g l(-1)。原子力显微镜和动态光散射研究表明胶束呈球形,平均直径为41.43 nm。研究了mPEG - PA在纳米载体核心中包封强效化学预防剂姜黄素的效用。将高度疏水的化合物如姜黄素包封在纳米载体中可使药物在水性体系中易于溶解,这可以增加给药的便利性并使静脉给药成为可能。载药胶束纳米颗粒在生理条件(pH 7.4)、模拟胃液(pH 1.2)和模拟肠液(pH 6.8)中表现出良好的稳定性。如使用纯脂肪酶和HeLa细胞裂解物进行的体外酶催化药物释放所表明的,这种胶束制剂可以用作酶触发的药物释放载体。游离姜黄素和包封姜黄素的IC(50)分别为14.32和15.58 microM。

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