Tityustoxin K alpha blocks voltage-gatednoninactivating K+ channels and unblocks inactivating K+ channels blocked byalpha-dendrotoxin in synaptosomes.
- 15 February 1994
- journal article
- research article
- Published by Proceedings of the National Academy of Sciences in Proceedings of the National Academy of Sciences
- Vol. 91 (4) , 1475-1479
- https://doi.org/10.1073/pnas.91.4.1475
Abstract
Two nonhomologous polypeptide toxins, tityustoxin K alpha (TsTX-K alpha) and tityustoxin K beta (TsTX-K beta), purified from the venom of the Brazilian scorpion Tityus serrulatus, selectively block voltage-gated noninactivating K+ channels in synaptosomes (IC50 values of 8 nM and 30 nM, respectively). In contrast, alpha-dendrotoxin (alpha-DTX) and charybdotoxin (ChTX) block voltage-gated inactivating K+ channels in synaptosomes (IC50 values of 90 nM and 40 nM, respectively). We studied interactions among these toxins in 125I-alpha-DTX binding and 86Rb efflux experiments. Both TsTX-K alpha and ChTX completely displaced specifically bound 125I-alpha-DTX from synaptic membranes, but TsTX-K beta had no effect on bound alpha-DTX. TsTX-K alpha and TsTX-K beta blocked the same noninactivating component of 100 mM K(+)-stimulated 86Rb efflux in synaptosomes. Both alpha-DTX and ChTX blocked the same inactivating component of the K(+)-stimulated 86Rb efflux in synaptosomes. Both the inactivating and the noninactivating components of the 100 mM K(+)-stimulated 86Rb efflux were completely blocked when 200 nM TsTX-K beta and either 600 nM alpha-DTX or 200 nM ChTX were present. The effects of TsTX-K alpha and ChTX on 86Rb efflux were also additive. When TsTX-K alpha was added in the presence of alpha-DTX, however, only the noninactivating component of the K(+)-stimulated efflux was blocked. The inactivating component could then be blocked by ChTX, which is structurally homologous to TsTX-K alpha. We conclude that TsTX-K alpha unblocks the voltage-gated inactivating K+ channels in synaptosomes when they are blocked by alpha-DTX, but not when they are blocked by ChTX. TsTX-K alpha binds to a site on the inactivating K+ channel that does not occlude the pore; its binding apparently prevents alpha-DTX (7054 Da), but not ChTX (4300 Da), from blocking the pore. The effects of TsTX-K alpha on 125I-alpha-DTX binding and 86Rb efflux are mimicked by noxiustoxin, which is homologous to TsTX-K alpha and ChTX.Keywords
This publication has 27 references indexed in Scilit:
- Dendrotoxins: Snake toxins that block potassium channels and facilitate neurotransmitter releasePublished by Elsevier ,2002
- Charybdotoxin blocks dendrotoxin‐sensitive voltage‐activated K+ channelsFEBS Letters, 1989
- Charybdotoxin blocks both Ca‐activated K channels and Ca‐independent voltage‐gated K channels in rat brain synaptosomesFEBS Letters, 1989
- An emerging pharmacology of peptide toxins targeted against potassium channelsThe Journal of Membrane Biology, 1988
- 4 POLYPEPTIDE COMPONENTS OF GREEN MAMBA VENOM SELECTIVELY BLOCK CERTAIN POTASSIUM CHANNELS IN RAT-BRAIN SYNAPTOSOMES1988
- Purification and characterization of a unique, potent inhibitor of apamin binding from Leiurus quinquestriatus hebraeus venom.Journal of Biological Chemistry, 1988
- Purification, sequence, and model structure of charybdotoxin, a potent selective inhibitor of calcium-activated potassium channels.Proceedings of the National Academy of Sciences, 1988
- Charybdotoxin and noxiustoxin, two homologous peptide inhibitors of the K+(Ca2+) channelFEBS Letters, 1988
- Potassium channels in isolated presynaptic nerve terminals from rat brain.The Journal of Physiology, 1985
- Charybdotoxin, a protein inhibitor of single Ca2+-activated K+ channels from mammalian skeletal muscleNature, 1985