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膜活性阳离子肽内化、溶血、细胞毒性和抗菌作用的比较分析:实验设置方面

Comparative analysis of internalisation, haemolytic, cytotoxic and antibacterial effect of membrane-active cationic peptides: aspects of experimental setup.

作者信息

Horváti Kata, Bacsa Bernadett, Mlinkó Tamás, Szabó Nóra, Hudecz Ferenc, Zsila Ferenc, Bősze Szilvia

机构信息

MTA-ELTE Research Group of Peptide Chemistry, Hungarian Academy of Sciences, Pázmány P. stny. 1/A, Budapest, 1117, Hungary.

Laboratory of Bacteriology, Korányi National Institute for Tuberculosis and Respiratory Medicine, Budapest, Hungary.

出版信息

Amino Acids. 2017 Jun;49(6):1053-1067. doi: 10.1007/s00726-017-2402-9. Epub 2017 Mar 17.

DOI:10.1007/s00726-017-2402-9
PMID:28314993
Abstract

Cationic peptides proved fundamental importance as pharmaceutical agents and/or drug carrier moieties functioning in cellular processes. The comparison of the in vitro activity of these peptides is an experimental challenge and a combination of different methods, such as cytotoxicity, internalisation rate, haemolytic and antibacterial effect, is necessary. At the same time, several issues need to be addressed as the assay conditions have a great influence on the measured biological effects and the experimental setup needs to be optimised. Therefore, critical comparison of results from different assays using representative examples of cell penetrating and antimicrobial peptides was performed and optimal test conditions were suggested. Our main goal was to identify carrier peptides for drug delivery systems of antimicrobial drug candidates. Based on the results of internalisation, haemolytic, cytotoxic and antibacterial activity assays, a classification of cationic peptides is advocated. We found eight promising carrier peptides with good penetration ability of which Penetratin, Tat, Buforin and Dhvar4 peptides showed low adverse haemolytic effect. Penetratin, Transportan, Dhvar4 and the hybrid CM15 peptide had the most potent antibacterial activity on Streptococcus pneumoniae (MIC lower than 1.2 μM) and Transportan was effective against Mycobacterium tuberculosis as well. The most selective peptide was the Penetratin, where the effective antimicrobial concentration on pneumococcus was more than 250 times lower than the HC value. Therefore, these peptides and their analogues will be further investigated as drug delivery systems for antimicrobial agents.

摘要

阳离子肽作为药物制剂和/或在细胞过程中发挥作用的药物载体部分具有至关重要的意义。比较这些肽的体外活性是一项实验挑战,需要结合不同的方法,如细胞毒性、内化率、溶血和抗菌作用。同时,由于测定条件对所测量的生物学效应有很大影响,且实验设置需要优化,因此有几个问题需要解决。因此,使用细胞穿透肽和抗菌肽的代表性实例对不同测定结果进行了批判性比较,并提出了最佳测试条件。我们的主要目标是为抗菌候选药物的药物递送系统鉴定载体肽。基于内化、溶血、细胞毒性和抗菌活性测定的结果,提倡对阳离子肽进行分类。我们发现了八种具有良好穿透能力的有前景的载体肽,其中穿膜肽、Tat、蟾蜍抗菌肽和Dhvar4肽表现出较低的不良溶血效应。穿膜肽、转运蛋白、Dhvar4和杂合CM15肽对肺炎链球菌具有最强的抗菌活性(最低抑菌浓度低于1.2μM),转运蛋白对结核分枝杆菌也有效。最具选择性的肽是穿膜肽,其对肺炎球菌的有效抗菌浓度比溶血浓度低250倍以上。因此,这些肽及其类似物将作为抗菌剂的药物递送系统进一步研究。

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