Analysis of the interacting surface of maurotoxin with the voltage‐gated Shaker B K⁺ channel

Abstract: Maurotoxin (MTX) is a 34-residue toxin that was isolated initially from the venom of the scorpion Scorpio maurus palmatus. Unlike the other toxins of the α-KTx6 family (Pi1, Pi4, Pi7, and HsTx1), MTX exhibits a unique disulfide bridge organization of the type C(1) C(5) , C(2) C(6) , C(3) C(4) , and C(7) C(8) (instead of the conventional C(1) C(5) , C(2) C(6) , C(3) C(7) , and C(4) C(8) , herein referred to as Pi1-like) that does not prevent its folding along the classic α/β scaffold of scorpion toxins.… Show more

“…Due to the unique selectivity profile of MTx for Kv1.2 and IK Ca , a number of experimental [5], [6], [7], [11], [12], [13], [14], [15] as well as theoretical [16], [17], [18] studies have been carried out to understand the binding modes of MTx to K + channels. These studies are consistent with Lys23 of MTx being the key residue which protrudes into the selectivity filter of Kv1.2 on binding.…”

Structural Basis of the Selective Block of Kv1.2 by Maurotoxin from Computer Simulations

“…Due to the unique selectivity profile of MTx for Kv1.2 and IK Ca , a number of experimental [5], [6], [7], [11], [12], [13], [14], [15] as well as theoretical [16], [17], [18] studies have been carried out to understand the binding modes of MTx to K + channels. These studies are consistent with Lys23 of MTx being the key residue which protrudes into the selectivity filter of Kv1.2 on binding.…”

Structural Basis of the Selective Block of Kv1.2 by Maurotoxin from Computer Simulations