Antimicrobial peptides (AMPs) are a potential alternative to classical antibiotics that are yet to achieve a therapeutic breakthrough for treatment of systemic infections. The antibacterial potency of pleurocidin, an AMP from Winter Flounder, is linked to its ability to cross bacterial plasma membranes and seek intracellular targets while also causing membrane damage. Here we describe modification strategies that generate pleurocidin analogues with substantially improved, broad spectrum, antibacterial properties, which are effective in murine models of bacterial lung infection. Increasing peptide-lipid intermolecular hydrogen bonding capabilities enhances conformational flexibility, associated with membrane translocation, but also membrane damage and potency, most notably against Gram-positive bacteria. This negates their ability to metabolically adapt to the AMP threat. An analogue comprising D-amino acids was well tolerated at an intravenous dose of 15âmg/kg and similarly effective as vancomycin in reducing EMRSA-15 lung CFU. This highlights the therapeutic potential of systemically delivered, bactericidal AMPs.
A pleurocidin analogue with greater conformational flexibility, enhanced antimicrobial potency and in vivo therapeutic efficacy.
一种具有更大构象灵活性、增强抗菌效力和体内治疗功效的侧耳素类似物
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作者:Manzo Giorgia, Hind Charlotte K, Ferguson Philip M, Amison Richard T, Hodgson-Casson Alice C, Ciazynska Katarzyna A, Weller Bethany J, Clarke Maria, Lam Carolyn, Man Rico C H, Shaughnessy Blaze G O', Clifford Melanie, Bui Tam T, Drake Alex F, Atkinson R Andrew, Lam Jenny K W, Pitchford Simon C, Page Clive P, Phoenix David A, Lorenz Christian D, Sutton J Mark, Mason A James
| 期刊: | Communications Biology | 影响因子: | 5.100 |
| 时间: | 2020 | 起止号: | 2020 Nov 27; 3(1):697 |
| doi: | 10.1038/s42003-020-01420-3 | 研究方向: | 其它 |
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