Synthetic ShK-like Peptide from the Jellyfish Nemopilema nomurai Has Human Voltage-Gated Potassium-Channel-Blocking Activity

Authors
Kim, Ye-JiJo, YejinLee, Seung EunKim, JungeunChoi, Jae-PilLee, NayoungWon, HyokyoungWoo, Dong HoYum, Seungshic
Issue Date
2024-05
Publisher
Multidisciplinary Digital Publishing Institute (MDPI)
Citation
Marine Drugs, v.22, no.5
Abstract
We identified a new human voltage-gated potassium channel blocker, NnK-1, in the jellyfish Nemopilema nomurai based on its genomic information. The gene sequence encoding NnK-1 contains 5408 base pairs, with five introns and six exons. The coding sequence of the NnK-1 precursor is 894 nucleotides long and encodes 297 amino acids containing five presumptive ShK-like peptides. An electrophysiological assay demonstrated that the fifth peptide, NnK-1, which was chemically synthesized, is an effective blocker of hKv1.3, hKv1.4, and hKv1.5. Multiple-sequence alignment with cnidarian Shk-like peptides, which have Kv1.3-blocking activity, revealed that three residues ((3)Asp, (25)Lys, and (34)Thr) of NnK-1, together with six cysteine residues, were conserved. Therefore, we hypothesized that these three residues are crucial for the binding of the toxin to voltage-gated potassium channels. This notion was confirmed by an electrophysiological assay with a synthetic peptide (NnK-1 mu) where these three peptides were substituted with (3)Glu, (25)Arg, and (34)Met. In conclusion, we successfully identified and characterized a new voltage-gated potassium channel blocker in jellyfish that interacts with three different voltage-gated potassium channels. A peptide that interacts with multiple voltage-gated potassium channels has many therapeutic applications in various physiological and pathophysiological contexts.
Keywords
TOXIN; KV1.3; INHIBITOR; TARGET; toxin; venom; jellyfish; Cnidaria; genomic information; electrophysiology
URI
https://pubs.kist.re.kr/handle/201004/150035
DOI
10.3390/md22050217
Appears in Collections:
KIST Article > 2024
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