Chemistry:OdK2

OdK2 - Swiss-model
Identifiers
Class	Small Proteins
Superfamily	Scorpion toxin-like
Family	Scorpion short chain toxin, potassium channel inhibitor
Protein	P0C909
Species	Odontobuthus doriae
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OdK2 is a toxin found in the venom of the Iranian scorpion Odonthobuthus doriae. It belongs to the α-KTx family, and selectively blocks the voltage-gated potassium channel Kv1.3 (KCNA3).

Etymology

Odonthobuthus doriae is a scorpion species that belongs to the Buthidae family, mainly found in central and southern Iran. OdK2 is an acronym indicating the toxins originating species, the type of ion channel it targets and the chronological order of its discovery.^[1] OdK1 was the first toxin isolated from the same species’ venom, targeting the Kv1.2 channel (KCNA2).^[2]

Chemistry

OdK2 is a relatively small peptide with 38 amino acids and a monoisotopic mass of 4079.869 Da (C₁₆₇H₂₇₈N₅₄O₄₉S₈).^[1]

OdK2-Disulphide bonds marked. Cys8-Cys-28, Cys14-Cys-33, Cys18-Cys-35 Swiss-model, P0C909

According to the unified nomenclature for short-chain peptides isolated from scorpion venoms, Odk2 can be classified in the second α-KTx family, selectively blocking voltage-gated potassium channels.^[3]

OdK2 is further classified as α-KTx 3.11 as it presents significant sequence homology with toxins from the α-KTx 3.x sub-family, especially Bs6, Agitoxin and Kaliotoxin.^[1] This fact suggests that frequently observed structural motifs present on other toxins of the same subfamily, such as the α/β scaffold and the typical disulfide pairing, can be assumed for OdK2 as well.^[1][4][5]

The presence of Lys27 and Phe25 residues, crucial for the α-KTx3-Kv1.3 interaction, is another highly conserved feature among α-KTx toxins.^[5]

Mode of action

OdK2 is one of the many Kv1.3 channel blockers found in the scorpion’s venom.^[1] There is evidence suggesting that their binding mechanism to Kv1.3 is governed by electrostatic forces, exerted between specific amino acid residues in the toxins and in the pore regions of the channel’s subunits.^[6] However, the precise OdK2 blocking mechanism remains unknown.^[1]

Two prominent features of OdK2 are its blocking potency (IC₅₀ value of 7.27 ± 2.7 nM) and its high selectivity for Kv1.3 channels, illustrated by 95% inhibition at a concentration of 35 nM, but no observed effect in other voltage-gated potassium channels. Amino acid residues only found in Kv1.3 pore regions and not in other Kv1.x channel family members, could potentially explain the high selectivity of OdK2.^[1]

Kv1.3 channels are delayed rectifier channels. Their main function is to repolarize the membrane, counterbalancing the depolarizing effect of calcium influx. As the precise modulation of intracellular calcium concentration is critical for the cell's activation and proliferation, occlusion of the potassium channels has a strong effect on the cell’s calcium signaling pathway, indirectly disrupting its normal function.^[7][8]

Toxicity

Observed effects of OdK2 infection include local pain, muscle paralysis and may lead to inflammation and necrosis.^[1]

References

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