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广泛的酪蛋白 A 和 B 的操作强调了这些抗菌肽对变化的耐受性。

Extensive manipulation of caseicins A and B highlights the tolerance of these antimicrobial peptides to change.

机构信息

Microbiology Department, University College Cork, Cork, Ireland.

出版信息

Appl Environ Microbiol. 2012 Apr;78(7):2353-8. doi: 10.1128/AEM.07312-11. Epub 2012 Jan 13.

Abstract

Caseicins A and B are low-molecular-weight antimicrobial peptides which are released by proteolytic digestion of sodium caseinate. Caseicin A (IKHQGLPQE) is a nine-amino-acid cationic peptide, and caseicin B (VLNENLLR) is a neutral eight-amino-acid peptide; both have previously been shown to exhibit antibacterial activity against a number of pathogens, including Cronobacter sakazakii. Previously, four variants of each caseicin which differed subtly from their natural counterparts were generated by peptide synthesis. Antimicrobial activity assays revealed that the importance of a number of the residues within the peptides was dependent on the strain being targeted. In this study, this engineering-based approach was expanded through the creation of a larger collection of 26 peptides which are altered in a variety of ways. The investigation highlights the generally greater tolerance of caseicin B to change, the fact that changes have a more detrimental impact on anti-Gram-negative activity, and the surprising number of variants which exhibit enhanced activity against Staphylococcus aureus.

摘要

-caseicins A 和 B 是低分子量的抗菌肽,通过对酪蛋白酸钠的蛋白水解消化释放出来。caseicin A(IKHQGLPQE)是一种九个氨基酸的阳离子肽,caseicin B(VLNENLLR)是一种中性的八个氨基酸的肽;两者都表现出对许多病原体的抗菌活性,包括阪崎克罗诺杆菌。以前,通过肽合成生成了每种 caseicin 的四个变体,它们与天然对应物略有不同。抗菌活性测定表明,肽内的许多残基的重要性取决于目标菌株。在这项研究中,通过创建一个更大的 26 种肽的集合,通过各种方式进行改变,扩展了基于工程的方法。该研究突出了 caseicin B 通常对变化的更大耐受性,以及变化对抗革兰氏阴性活性的更不利影响,以及令人惊讶的数量的变体对金黄色葡萄球菌表现出增强的活性。

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