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Cited 2 time in webofscience Cited 2 time in scopus
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N-type Ca-v channel inhibition by spider venom peptide of Argiope bruennichi

Authors
Hwang, In-WookShin, Min KyoungLee, Yoo-JungKim, Seung TaeLee, Sue YeonLee, ByungjoJang, WonheeYeo, Joo-HongLee, SeungkiSung, Jung-Suk
Issue Date
Jan-2021
Publisher
KOREAN SOCIETY TOXICOGENOMICS & TOXICOPROTEOMICS-KSTT
Keywords
Spider venom; Argiope bruennichi; Transcriptomics; RNA-sequencing; In silico analysis; Neurotoxicity
Citation
MOLECULAR & CELLULAR TOXICOLOGY, v.17, no.1, pp 59 - 67
Pages
9
Indexed
SCIE
SCOPUS
KCI
Journal Title
MOLECULAR & CELLULAR TOXICOLOGY
Volume
17
Number
1
Start Page
59
End Page
67
URI
https://scholarworks.dongguk.edu/handle/sw.dongguk/5503
DOI
10.1007/s13273-020-00109-2
ISSN
1738-642X
2092-8467
Abstract
Background The spider venom is composed of various bioactive peptides and has well-known physiological characteristics, such as cytolytic and neurotoxic activities. However, there have been few studies on neurotoxic peptides derived from domestic indigenous spiders in Korea. Objective The study aimed to characterize and identify the venom peptide through genomic analysis from the domestic indigenous spider, Argiope bruennichi. Toxin-like peptides were selected using homology analysis against well-known toxin peptides along with the secondary structural characterization analysis by cysteine pattern and disulfide bonds. Modulation of voltage-gated calcium (Ca-v) channel was measured by Ca2+ influx using fluorescence dye. Results We found that a novel peptide Aranetoxin-Ab1a significantly reduced intracellular Ca2+ levels in human neuroblastoma cell line SH-SY5Y via the inactivation of N-type Ca-v channels. Decreased intracellular Ca2+ influx by the treatment of the peptide inactivated the extracellular-regulated protein kinase 1/2 and cAMP-response factor binding protein pathway. Conclusion Our results provide beneficial information for the potential development of drugs utilizing novel peptide derived from spider venom, showing the inhibition of N-type Ca-v by the peptide.
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