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光致变色二芳烯基 β-发夹肽作为溶膜性抗菌和抗癌剂的结构-活性关系。

Structure-Activity Relationships of Photoswitchable Diarylethene-Based β-Hairpin Peptides as Membranolytic Antimicrobial and Anticancer Agents.

机构信息

Institute of Biological Interfaces (IBG-2) , Karlsruhe Institute of Technology (KIT) , POB 3640, 76021 Karlsruhe , Germany.

Institute of High Technologies , Taras Shevchenko National University of Kyiv , Vul. Volodymyrska 60 , 01601 Kyiv , Ukraine.

出版信息

J Med Chem. 2018 Dec 13;61(23):10793-10813. doi: 10.1021/acs.jmedchem.8b01428. Epub 2018 Dec 4.

Abstract

Five series (28 structures) of photoswitchable β-hairpin peptides were synthesized based on the cyclic scaffold of the natural antibiotic gramicidin S. Cell-type selectivity was compared for all activated (diarylethene "ring-open") and deactivated ("ring-closed") forms in terms of antibacterial activity (MIC against Escherichia coli and Bacillus subtilis), anticancer activity (IC against HeLa cell line), and hemolytic cytotoxicity (HC against human erythrocytes). Correlations between the conformational plasticity of the peptides, their hydrophobicity, and their bioactivity were also analyzed. Considerable improvements in selectivity were achieved compared to the reference compound. We found a dissociation of the anticancer activity from hemolysis. Phototherapeutic indices (PTI), HC(closed)/MIC(open) and HC(closed)/IC(open), were introduced for the peptides as safety criteria. The highest PTI for HeLa-selective toxicity were observed among analogues containing hydroxyleucine on the hydrophobic face. For one compound, high PTIs were demonstrated across a range of different cancer cell lines, including a doxorubicin-resistant one.

摘要

基于天然抗生素短杆菌肽 S 的环状支架,合成了五个系列(28 个结构)的光致变色β发夹肽。根据抗菌活性(对大肠杆菌和枯草芽孢杆菌的 MIC)、抗癌活性(对 HeLa 细胞系的 IC)和溶血细胞毒性(对人红细胞的 HC),比较了所有激活(二芳基乙烯“开环”)和失活(“闭环”)形式的细胞类型选择性。还分析了肽的构象灵活性、疏水性与其生物活性之间的相关性。与参考化合物相比,选择性得到了显著提高。我们发现抗癌活性与溶血分离。为肽引入了光治疗指数(PTI),HC(闭合)/MIC(开环)和 HC(闭合)/IC(开环),作为安全标准。在疏水面上含有羟基亮氨酸的类似物中观察到对 HeLa 选择性毒性的最高 PTI。对于一种化合物,在一系列不同的癌细胞系中,包括多柔比星耐药细胞系,均表现出较高的 PTI。

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