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External lysis of Escherichia coli by a bacteriophage endolysin modified with hydrophobic amino acids

机译:疏水性氨基酸修饰的噬菌体内溶素对大肠杆菌的外部裂解

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摘要

Drug-resistant bacteria are a serious threat to global public health. Gram-positive bacterial endolysin preparations have been successfully used to fight Gram-positive bacteria as a novel antimicrobial replacement strategy. However, Gram-negative bacterial phage endolysins cannot be applied directly to destroy Gram-negative strains due to the externally inaccessible peptidoglycan layer of the cell wall; this has seriously hampered the development of endolysin-like antibiotics against Gram-negative bacteria. In this study, 3–12 hydrophobic amino acids were successively added to the C-terminus of Escherichia coli phage endolysin Lysep3 to create five different hydrophobic-modified endolysins. Compared with endogenous Lysep3, endolysins modified with hydrophobic amino acids surprisingly could kill E. coli from outside of the cell at the appropriate pH and endolysin concentration. The lysis ability of modified endolysins were enhanced with increasing numbers of hydrophobic amino acids at the C-terminus of endolysin. Thus, these findings demonstrate that the enhancement of hydrophobicity at the C-terminus enables the endolysin to act upon E. coli from the outside, representing a novel method of lysing Gram-negative antibiotic-resistant bacteria.
机译:耐药细菌是对全球公共健康的严重威胁。革兰氏阳性细菌内溶素制剂已成功用于对抗革兰氏阳性细菌,这是一种新型的抗菌药物替代策略。然而,由于细胞壁的外部肽聚糖层无法进入,革兰氏阴性细菌噬菌体溶素不能直接用于破坏革兰氏阴性菌株。这严重阻碍了针对革兰氏阴性菌的内溶素类抗生素的开发。在这项研究中,将3–12个疏水氨基酸顺序添加到大肠杆菌噬菌体溶素Lysep3的C末端,以创建5种不同的疏水修饰的溶素。与内源性Lysep3相比,在适当的pH和内溶素浓度下,疏水性氨基酸修饰的内溶素出人意料地可以杀死细胞外的大肠杆菌。修饰的细胞内溶素的裂解能力随细胞内溶素C端疏水性氨基酸数目的增加而增强。因此,这些发现表明,C末端疏水性的增强使得内溶素能够从外部作用于大肠杆菌,代表了裂解革兰氏阴性抗生素抗性细菌的新方法。

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