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Cited 6 time in webofscience Cited 6 time in scopus
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The Identification of a Novel Spider Toxin Peptide, Lycotoxin-Pa2a, with Antibacterial and Anti-Inflammatory Activitiesopen access

Authors
Shin, Min KyoungHwang, In-WookJang, Bo-YoungBu, Kyung-BinHan, Dong-HeeLee, Seung-HoOh, Jin WookYoo, Jung SunSung, Jung-Suk
Issue Date
Dec-2023
Publisher
MDPI
Keywords
in silico analysis; spider venom transcriptome; spider toxin peptide; antimicrobial activity; anti-inflammatory activity
Citation
Antibiotics, v.12, no.12, pp 1 - 18
Pages
18
Indexed
SCIE
SCOPUS
Journal Title
Antibiotics
Volume
12
Number
12
Start Page
1
End Page
18
URI
https://scholarworks.dongguk.edu/handle/sw.dongguk/20807
DOI
10.3390/antibiotics12121708
ISSN
2079-6382
2079-6382
Abstract
With the increasing challenge of controlling infectious diseases due to the emergence of antibiotic-resistant strains, the importance of discovering new antimicrobial agents is rapidly increasing. Animal venoms contain a variety of functional peptides, making them a promising platform for pharmaceutical development. In this study, a novel toxin peptide with antibacterial and anti-inflammatory activities was discovered from the spider venom gland transcriptome by implementing computational approaches. Lycotoxin-Pa2a (Lytx-Pa2a) showed homology to known-spider toxin, where functional prediction indicated the potential of both antibacterial and anti-inflammatory peptides without hemolytic activity. The colony-forming assay and minimum inhibitory concentration test showed that Lytx-Pa2a exhibited comparable or stronger antibacterial activity against pathogenic strains than melittin. Following mechanistic studies revealed that Lytx-Pa2a disrupts both cytoplasmic and outer membranes of bacteria while simultaneously inducing the accumulation of reactive oxygen species. The peptide exerted no significant toxicity when treated to human primary cells, murine macrophages, and bovine red blood cells. Moreover, Lytx-Pa2a alleviated lipopolysaccharide-induced inflammation in mouse macrophages by suppressing the expression of inflammatory mediators. These findings not only suggested that Lytx-Pa2a with dual activity can be utilized as a new antimicrobial agent for infectious diseases but also demonstrated the implementation of in silico methods for discovering a novel functional peptide, which may enhance the future utilization of biological resources.
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