Selective block of human Kv1.1 channels and an epilepsy-associated gain-of-function mutation by AETX-K peptide.
Ruiming ZhaoArwa QasimPunyanuch SophanpanichkulHui DaiMahasweta NayakInbal SherJordan H ChillSteven A N GoldsteinPublished in: FASEB journal : official publication of the Federation of American Societies for Experimental Biology (2023)
Dysfunction of the human voltage-gated K + channel Kv1.1 has been associated with epilepsy, multiple sclerosis, episodic ataxia, myokymia, and cardiorespiratory dysregulation. We report here that AETX-K, a sea anemone type I (SAK1) peptide toxin we isolated from a phage display library, blocks Kv1.1 with high affinity (K i ~ 1.6 pM) and notable specificity, inhibiting other Kv channels we tested a million-fold less well. Nuclear magnetic resonance (NMR) was employed both to determine the three-dimensional structure of AETX-K, showing it to employ a classic SAK1 scaffold while exhibiting a unique electrostatic potential surface, and to visualize AETX-K bound to the Kv1.1 pore domain embedded in lipoprotein nanodiscs. Study of Kv1.1 in Xenopus oocytes with AETX-K and point variants using electrophysiology demonstrated the blocking mechanism to employ a toxin-channel configuration we have described before whereby AETX-K Lys 23 , two positions away on the toxin interaction surface from the classical blocking residue, enters the pore deeply enough to interact with K + ions traversing the pathway from the opposite side of the membrane. The mutant channel Kv1.1-L 296 F is associated with pharmaco-resistant multifocal epilepsy in infants because it significantly increases K + currents by facilitating opening and slowing closure of the channels. Consistent with the therapeutic potential of AETX-K for Kv1.1 gain-of-function-associated diseases, AETX-K at 4 pM decreased Kv1.1-L 296 F currents to wild-type levels; further, populations of heteromeric channels formed by co-expression Kv1.1 and Kv1.2, as found in many neurons, showed a K i of ~10 nM even though homomeric Kv1.2 channels were insensitive to the toxin (K i > 2000 nM).
Keyphrases
- image quality
- dual energy
- magnetic resonance
- escherichia coli
- multiple sclerosis
- computed tomography
- endothelial cells
- wild type
- gene expression
- body composition
- particulate matter
- oxidative stress
- signaling pathway
- spinal cord
- spinal cord injury
- contrast enhanced
- heavy metals
- quantum dots
- human health
- tissue engineering
- structural basis