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Determination of Essential and Variable Residues in Pediocin PA-1 by NNK Scanning†

机译:NNK扫描测定Pediocin PA-1中的必需和可变残留†

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摘要

Pediocin PA-1 is an antimicrobial peptide (called bacteriocin) that shows inhibitory activity against the food-borne pathogen Listeria monocytogenes. To elucidate which residue(s) is responsible for this function, the antimicrobial activities of pediocin PA-1 mutants were evaluated and compared. Each of the 44 native codons was replaced with the NNK triplet oligonucleotide in a technique termed NNK scanning, and 35 mutations at each position were examined for antimicrobial activities using a modified colony overlay screening method. As a consequence, the functional responsibility of each residue was estimated by counting the number of active mutants, allowing us to identify candidate essential/variable residues. Activity was abrogated by many of the mutations at residues Y2, G6, C9, C14, C24, W33, G37, and C44, indicating that these residues may be essential. In contrast, activity was retained by almost all versions harboring mutations at K1, T8, G10, S13, G19, N28, and N41, indicating that these are functionally redundant residues. Sequence analysis revealed that only the wild type was active and 14 and 11 substitutions were inactive at G6 and C14, respectively, while 12 and 11 substitutions were active and 2 and 0 substitutions were inactive at T8 and K1, respectively. These findings suggest that NNK scanning is effective for determining essential and variable residues in pediocin PA-1, leading to an elucidation of structure-function relationships and to improvements in the antimicrobial function efficiently by peptide engineering.
机译:Pediocin PA-1是一种抗菌肽(称为细菌素),对食源性单核细胞增生李斯特氏菌具有抑制活性。为了阐明负责该功能的残基,评估并比较了pediocin PA-1突变体的抗菌活性。在称为NNK扫描的技术中,将44个天然密码子中的每一个替换为NNK三重态寡核苷酸,并使用改良的菌落覆盖筛选方法检查了每个位置的35个突变的抗菌活性。结果,通过计数活性突变体的数量来估计每个残基的功能责任,从而使我们能够鉴定候选的必需/可变残基。活性由于残基Y2,G6,C9,C14,C24,W33,G37和C44的许多突变而被废除,表明这些残基可能是必不可少的。相反,几乎所有具有K1,T8,G10,S13,G19,N28和N41突变的版本均保留了活性,表明这些是功能上的冗余残基。序列分析表明,只有野生型是有活性的,在G6和C14分别有14和11个取代是无效的,而在T8和K1处有12和11个取代是有活性的,而2和0取代是无活性的。这些发现表明,NNK扫描对于确定pediocin PA-1中的必需残基和可变残基是有效的,从而阐明了结构-功能关系并通过肽工程有效地改善了抗菌功能。

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