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源自FKCRRQWQWRMKKGLA序列的截短型和多价肽对大肠杆菌ATCC 25922和金黄色葡萄球菌ATCC 25923的抗菌活性

Antimicrobial Activity of Truncated and Polyvalent Peptides Derived from the FKCRRQWQWRMKKGLA Sequence against Escherichia coli ATCC 25922 and Staphylococcus aureus ATCC 25923.

作者信息

Huertas Nataly de Jesús, Monroy Zuly Jenny Rivera, Medina Ricardo Fierro, Castañeda Javier Eduardo García

机构信息

Chemistry Department, Universidad Nacional de Colombia, Bogotá Carrera 45 No. 26-85, Building 451, Office 409, Laboratory 334, Bogotá 11321, Colombia.

Pharmacy Department, Universidad Nacional de Colombia, Bogotá Carrera 45 No. 26-85, Building 450, office 203, Bogotá 11321, Colombia.

出版信息

Molecules. 2017 Jun 14;22(6):987. doi: 10.3390/molecules22060987.

Abstract

Peptides derived from LfcinB were designed and synthesized, and their antibacterial activity was tested against ATCC 25922 and ATCC 25923. Specifically, a peptide library was constructed by systemically removing the flanking residues (N or C-terminal) of Lfcin 17-31 (FKCRRWQWRMKKLGA), maintaining in all peptides the RRWQWR sequence that corresponds to the minimal antimicrobial motif. For this research, also included were (i) a peptide containing an Ala instead of Cys ([Ala]-LfcinB 17-31) and (ii) polyvalent peptides containing the RRWQWR sequence and a non-natural amino acid (aminocaproic acid). We established that the lineal peptides LfcinB 17-25 and LfcinB 17-26 exhibited the greatest activity against ATCC 25922 and ATCC 25923, respectively. On the other hand, polyvalent peptides, a dimer and a tetramer, exhibited the greatest antibacterial activity, indicating that multiple copies of the sequence increase the activity. Our results suggest that the dimeric and tetrameric sequence forms potentiate the antibacterial activity of lineal sequences that have exhibited moderate antibacterial activity.

摘要

设计并合成了源自乳铁蛋白B的肽段,并测试了它们对ATCC 25922和ATCC 25923的抗菌活性。具体而言,通过系统性去除乳铁蛋白17 - 31(FKCRRWQWRMKKLGA)的侧翼残基(N端或C端)构建了一个肽库,所有肽段都保留了与最小抗菌基序相对应的RRWQWR序列。在本研究中,还包括(i)一个用丙氨酸替代半胱氨酸的肽段([Ala]-LfcinB 17 - 31)和(ii)含有RRWQWR序列和一种非天然氨基酸(氨基己酸)的多价肽段。我们发现线性肽段LfcinB 17 - 25和LfcinB 17 - 26分别对ATCC 25922和ATCC 25923表现出最大活性。另一方面,多价肽段,即二聚体和四聚体,表现出最大的抗菌活性,这表明该序列的多个拷贝增加了活性。我们的结果表明,二聚体和四聚体序列形式增强了已表现出中等抗菌活性的线性序列的抗菌活性。

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