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新型自组装肽对疏水性抗癌药物的释放

Release of hydrophobic anticancer drug from a newly designed self-assembling peptide.

作者信息

Wu Min, Ye Zhaoyang, Liu Yanfei, Liu Bo, Zhao Xiaojun

机构信息

West China Hospital Nanomedicine Laboratory and Institute for Nanobiomedical Technology and Membrane Biology, West China Hospital, Sichuan University, Chengdu, 610041, P R China.

出版信息

Mol Biosyst. 2011 Jun;7(6):2040-7. doi: 10.1039/c0mb00271b. Epub 2011 Apr 14.

DOI:10.1039/c0mb00271b
PMID:21491031
Abstract

A newly designed self-assembling peptide, P4 (Ac-NH-LDLKLELKLDLKLELK-CONH(2)), capable of stabilizing hydrophobic compounds in aqueous solution has been discovered. The ionic self-complementary peptide P4 has 16 amino acids, ∼5 nm in size, with an alternating polar and non-polar pattern. Circular dichroism analysis demonstrated that P4 forms stable β-sheet structures, and self-assembles into nanofibers, which was demonstrated by atomic force microscopy. These nanofibers can form a scaffold hydrogel consisting of >99% water. It showed that the P4 hydrogel had stable hydrogel rheological properties. The ability of the peptide to stabilize the hydrophobic anticancer agent ellipticine was tested in this research. The results showed that the state of ellipticine in the complexes was dependent on the concentration of the peptide, which also affected the size and morphology of the complex. The anticancer activity of the complexes was studied by testing the viability with a MTT assay and a LIVE/DEAD Viability/Cytotoxicity kit in two cancer cell lines including SMMC7721 and EC9706. The viability results showed that complexes of protonated ellipticine could significantly reduce the viability of the two cell lines. The results described herein provide further incentives for basic studies on self-assembling peptide-based delivery of hydrophobic anticancer drugs.

摘要

一种新设计的自组装肽P4(Ac-NH-LDLKLELKLDLKLELK-CONH(2))被发现,它能够在水溶液中稳定疏水性化合物。离子自互补肽P4有16个氨基酸,大小约为5纳米,具有交替的极性和非极性模式。圆二色性分析表明,P4形成稳定的β-折叠结构,并自组装成纳米纤维,这通过原子力显微镜得到证实。这些纳米纤维可以形成一种由>99%的水组成的支架水凝胶。结果表明,P4水凝胶具有稳定的水凝胶流变学性质。本研究测试了该肽稳定疏水性抗癌药物椭圆玫瑰树碱的能力。结果表明,椭圆玫瑰树碱在复合物中的状态取决于肽的浓度,这也影响了复合物的大小和形态。通过使用MTT法和LIVE/DEAD活力/细胞毒性试剂盒在包括SMMC7721和EC9706的两种癌细胞系中测试活力,研究了复合物的抗癌活性。活力结果表明,质子化椭圆玫瑰树碱的复合物可显著降低两种细胞系的活力。本文所述结果为基于自组装肽的疏水性抗癌药物递送的基础研究提供了进一步的动力。

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