Novel Tarantula Toxins for Subtypes of Voltage-Dependent Potassium Channels in the Kv2 and Kv4 Subfamilies

Three novel peptides with the ability to inhibit voltage-dependent potassium channels in the shab (Kv2) and shal (Kv4) subfamilies were identified from the venom of the African tarantulas Stromatopelma calceata (ScTx1) and Heteroscodra maculata (HmTx1, HmTx2). The three toxins are 34- to 38-amino ac...

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Bibliographic Details
Published in:Molecular pharmacology 2002-07, Vol.62 (1), p.48-57
Main Authors: Escoubas, Pierre, Diochot, Sylvie, Célérier, Marie-Louise, Nakajima, Terumi, Lazdunski, Michel
Format: Article
Language:English
Subjects:
Amino Acid Sequence
Animals
Calcium - metabolism
Cerebellum - cytology
Cerebellum - metabolism
Delayed Rectifier Potassium Channels
Female
Molecular Sequence Data
Potassium Channels - metabolism
Potassium Channels, Voltage-Gated - classification
Potassium Channels, Voltage-Gated - metabolism
Rats
Rats, Wistar
Sequence Homology, Amino Acid
Shab Potassium Channels
Sodium Channels - metabolism
Spider Venoms - chemistry
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Summary:Three novel peptides with the ability to inhibit voltage-dependent potassium channels in the shab (Kv2) and shal (Kv4) subfamilies were identified from the venom of the African tarantulas Stromatopelma calceata (ScTx1) and Heteroscodra maculata (HmTx1, HmTx2). The three toxins are 34- to 38-amino acid peptides that belong to the structural family of inhibitor cystine knot spider peptides reticulated by three disulfide bridges. Electrophysiological recordings in COS cells show that these toxins act as gating modifier of voltage-dependent K + channels. ScTx1 is the first high-affinity inhibitor of the Kv2.2 channel subtype (IC 50 , 21.4 nM) to be described. ScTx1 also inhibits the Kv2.1 channels, with an IC 50 of 12.7 nM, and Kv2.1/Kv9.3 heteromultimers that have been proposed to be involved in O 2 sensing in pulmonary artery myocytes. In addition, it is the most effective inhibitor of Kv4.2 channels described thus far, with an IC 50 of 1.2 nM. HmTx toxins share sequence similarities with both the potassium channel blocker toxins (HmTx1) and the calcium channel blocker toxin ω-GsTx SIA (HmTx2). They inhibit potassium current associated with Kv2 subtypes in the 100 to 300 nM concentration range. HmTx2 seems to be a specific inhibitor of Kv2 channels, whereas HmTx1 also inhibits Kv4 channels, including Kv4.1, with the same potency. HmTx1 is the first described peptide effector of the Kv4.1 subtype. Those novel toxins are new tools for the investigation of the physiological role of the different potassium channel subunits in cellular physiology.
ISSN:0026-895X
1521-0111
DOI:10.1124/mol.62.1.48