2015
DOI: 10.1371/journal.pone.0119525
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Human β-Defensin 4 with Non-Native Disulfide Bridges Exhibit Antimicrobial Activity

Abstract: Human defensins play multiple roles in innate immunity including direct antimicrobial killing and immunomodulatory activity. They have three disulfide bridges which contribute to the stability of three anti-parallel β-strands. The exact role of disulfide bridges and canonical β-structure in the antimicrobial action is not yet fully understood. In this study, we have explored the antimicrobial activity of human β-defensin 4 (HBD4) analogs that differ in the number and connectivity of disulfide bridges. The cyst… Show more

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Cited by 36 publications
(30 citation statements)
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“…Given that indolicidin induces local thinning of the bilayer ; these formations are likely vesicles formed from phospholipids of the cell's membrane and containing part of the intracellular material. Similar images were obtained by confocal microscopy of E. coli treated with human beta‐defensins‐4 modified by introducing disulfide bridges .…”
Section: Resultssupporting
confidence: 61%
“…Given that indolicidin induces local thinning of the bilayer ; these formations are likely vesicles formed from phospholipids of the cell's membrane and containing part of the intracellular material. Similar images were obtained by confocal microscopy of E. coli treated with human beta‐defensins‐4 modified by introducing disulfide bridges .…”
Section: Resultssupporting
confidence: 61%
“…Also, the proportion of hydrophobic groups in the surface is quite similar in most defensins, ranging from 45% to 65%. Thus, the ability of β‐defensins to interact with microbial membranes is determined more by the ratio of polar to hydrophobic residues on the peptide surface or by the total positive charge, rather than by their individual primary structures or three‐dimensional structures, with the β‐defensin fold or disulfide pattern not being mandatory for antimicrobial activity . Even though these common features are required for antimicrobial activity, structure analyses have failed to detect a common pattern of amino acidic residues for the distribution of polar and hydrophobic residues on the surface of β‐defensins .…”
Section: Resultsmentioning
confidence: 99%
“…Thus, the ability of β-defensins to interact with microbial membranes is determined more by the ratio of polar to hydrophobic residues on the peptide surface or by the total positive charge, rather than by their individual primary structures or three-dimensional structures, with the β-defensin fold or disulfide pattern not being mandatory for antimicrobial activity. 41,48,49,51,53,54 Even though these common features are required for antimicrobial activity, structure analyses have failed to detect a common pattern of amino acidic residues for the distribution of polar and hydrophobic residues on the surface of β-defensins. 41 However, minor differences in β-defensin structural features may be responsible for their specificity toward certain types of bacteria, fungi or protozoa.…”
Section: Peptide Preparationmentioning
confidence: 99%
“…Both CCL20 and HBD2 have antifungal properties, [40][41][42] and we next exposed whole skin biopsy specimens to fungal products. In line with our findings in primary keratinocytes, heat-killed C albicans increased CCL20 and DEFB4A/B expression in epidermis from NLP but not healthy epidermis (Fig 5, E).…”
Section: Epidermal Ccr6-expressing T Cells Are Effective With Regard mentioning
confidence: 99%