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Solution structure of HpTX2, a toxin from Heteropoda venatoria spider that blocks Kv4.2 potassium channel

Published online by Cambridge University Press:  15 December 2000

CÉDRIC BERNARD
Affiliation:
AFMB, CNRS UMR 6098, IFR1, 31, Chemin Joseph-Aiguier, 13402 Marseille Cedex 20, France
CHRISTIAN LEGROS
Affiliation:
Institut für Neurale Signalverarbeitung, ZMNH, Universität Hamburg, Martinistr. 52, D-20246 Hamburg, Germany
GILLES FERRAT
Affiliation:
AFMB, CNRS UMR 6098, IFR1, 31, Chemin Joseph-Aiguier, 13402 Marseille Cedex 20, France
ULRIKE BISCHOFF
Affiliation:
GENIONmbH, Absteistr. 57, D-20149 Hamburg, Germany
ANNETTE MARQUARDT
Affiliation:
Institut für Neurale Signalverarbeitung, ZMNH, Universität Hamburg, Martinistr. 52, D-20246 Hamburg, Germany
OLAF PONGS
Affiliation:
Institut für Neurale Signalverarbeitung, ZMNH, Universität Hamburg, Martinistr. 52, D-20246 Hamburg, Germany
HERVÉ DARBON
Affiliation:
AFMB, CNRS UMR 6098, IFR1, 31, Chemin Joseph-Aiguier, 13402 Marseille Cedex 20, France
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Abstract

HpTX2 is a toxin from the venom of Heteropoda venatoria spider that has been demonstrated to bind on Kv4.2 potassium channel. We have determined the solution structure of recombinant HpTX2 by use of conventional two-dimensional NMR techniques followed by distance-geometry and molecular dynamics. The calculated structure belongs to the Inhibitory Cystin Knot structural family that consists in a compact disulfide-bonded core, from which four loops emerge. A poorly defined two-stranded antiparallel β-sheet (residues 20–23 and 25–28) is detected. Analysis of the electrostatic charge anisotropy allows us to propose a functional map of HpTX2 different from the one described for κ-conotoxin PVIIA, but strongly related to the one of charybdotoxin. The orientation of the dipole moment of HpTX2 emerges through K27 which could therefore be the critical lysine residue. Close to this lysine are a second basic residue, R23, an aromatic cluster (F7, W25, W30) and an hydrophobic side chain (L24). The high density in aromatic side chains of the putative functional surface as well as the lack of an asparagine is proposed to be the structural basis of the specificity of HpTX2 toward Kv4.2 channel.

Type
Research Article
Information
Protein Science , Volume 9 , Issue 11 , November 2000 , pp. 2059 - 2067
Copyright
2000 The Protein Society

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