Phyla- and subtype-selectivity of CgNa, a Na+ channel toxin from the venom of the Giant Caribbean Sea Anemone Condylactis gigantea

Phyla- and subtype-selectivity of CgNa, a Na+ channel toxin from the venom of the Giant Caribbean Sea Anemone Condylactis gigantea

Because of their prominent role in electro-excitability, voltage-gated sodium (NaV) channels have become the foremost important target of animal toxins. These toxins have developed the ability to discriminate between closely related NaV subtypes, making them powerful tools to study NaV channel funct...

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Main Authors: Bert eBillen, Sarah eDebaveye, Lászlo eBéress, Anoland eGarateix, Jan eTytgat
Format: Article
Language:English
Published: Frontiers Media S.A. 2010-11-01
Series:Frontiers in Pharmacology
Subjects:
Selectivity
Sodium channel
Inactivation
toxin
sea anemone
subtype
Online Access:http://journal.frontiersin.org/Journal/10.3389/fphar.2010.00133/full
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spelling doaj-af7212d297c54b7eaf0e15e98133fb232020-11-24T23:06:47ZengFrontiers Media S.A.Frontiers in Pharmacology1663-98122010-11-01110.3389/fphar.2010.001337505Phyla- and subtype-selectivity of CgNa, a Na+ channel toxin from the venom of the Giant Caribbean Sea Anemone Condylactis giganteaBert eBillen0Sarah eDebaveye1Lászlo eBéress2Anoland eGarateix3Jan eTytgat4University of LeuvenUniversity of LeuvenMedical High School HannoverMinistry of Science, Technology and EnvirnnmentUniversity of LeuvenBecause of their prominent role in electro-excitability, voltage-gated sodium (NaV) channels have become the foremost important target of animal toxins. These toxins have developed the ability to discriminate between closely related NaV subtypes, making them powerful tools to study NaV channel function and structure. CgNa is a 47-amino acid residue type I toxin isolated from the venom of the giant Caribbean sea anemone Condylactis gigantea. Previous studies showed that this toxin slows the fast inactivation of TTX-sensitive voltage-gated sodium (NaV) currents in rat dorsal root ganglion neurons. To illuminate the underlying NaV subtype-selectivity pattern, we have assayed the effects of CgNa on a broad range of mammalian isoforms (NaV1.2–NaV1.8) expressed in Xenopus oocytes. This study demonstrates that CgNa selectively slows the fast inactivation of rNaV1.3/β1, mNaV1.6/β1 and, to a lesser extent, hNaV1.5/β1, while the other mammalian isoforms remain unaffected. Importantly, CgNa was also examined on the insect sodium channel DmNaV1/tipE, revealing a clear phyla-selectivity in the efficacious actions of the toxin. CgNa strongly inhibits the inactivation of the insect NaV channel, resulting in a dramatic increase in peak current amplitude and complete removal of fast and steady-state inactivation. Together with the previously determined solution structure, the subtype-selective effects revealed in this study make of CgNa an interesting pharmacological probe to investigate the functional role of specific NaV channel subtypes. Moreover, further structural studies could provide important information on the molecular mechanism of NaV channel inactivation.http://journal.frontiersin.org/Journal/10.3389/fphar.2010.00133/fullSelectivitySodium channelInactivationtoxinsea anemonesubtype
collection DOAJ
language English
format Article
sources DOAJ
author Bert eBillen
Sarah eDebaveye
Lászlo eBéress
Anoland eGarateix
Jan eTytgat
spellingShingle Bert eBillen
Sarah eDebaveye
Lászlo eBéress
Anoland eGarateix
Jan eTytgat
Phyla- and subtype-selectivity of CgNa, a Na+ channel toxin from the venom of the Giant Caribbean Sea Anemone Condylactis gigantea
Frontiers in Pharmacology
Selectivity
Sodium channel
Inactivation
toxin
sea anemone
subtype
author_facet Bert eBillen
Sarah eDebaveye
Lászlo eBéress
Anoland eGarateix
Jan eTytgat
author_sort Bert eBillen
title Phyla- and subtype-selectivity of CgNa, a Na+ channel toxin from the venom of the Giant Caribbean Sea Anemone Condylactis gigantea
title_short Phyla- and subtype-selectivity of CgNa, a Na+ channel toxin from the venom of the Giant Caribbean Sea Anemone Condylactis gigantea
title_full Phyla- and subtype-selectivity of CgNa, a Na+ channel toxin from the venom of the Giant Caribbean Sea Anemone Condylactis gigantea
title_fullStr Phyla- and subtype-selectivity of CgNa, a Na+ channel toxin from the venom of the Giant Caribbean Sea Anemone Condylactis gigantea
title_full_unstemmed Phyla- and subtype-selectivity of CgNa, a Na+ channel toxin from the venom of the Giant Caribbean Sea Anemone Condylactis gigantea
title_sort phyla- and subtype-selectivity of cgna, a na+ channel toxin from the venom of the giant caribbean sea anemone condylactis gigantea
publisher Frontiers Media S.A.
series Frontiers in Pharmacology
issn 1663-9812
publishDate 2010-11-01
description Because of their prominent role in electro-excitability, voltage-gated sodium (NaV) channels have become the foremost important target of animal toxins. These toxins have developed the ability to discriminate between closely related NaV subtypes, making them powerful tools to study NaV channel function and structure. CgNa is a 47-amino acid residue type I toxin isolated from the venom of the giant Caribbean sea anemone Condylactis gigantea. Previous studies showed that this toxin slows the fast inactivation of TTX-sensitive voltage-gated sodium (NaV) currents in rat dorsal root ganglion neurons. To illuminate the underlying NaV subtype-selectivity pattern, we have assayed the effects of CgNa on a broad range of mammalian isoforms (NaV1.2–NaV1.8) expressed in Xenopus oocytes. This study demonstrates that CgNa selectively slows the fast inactivation of rNaV1.3/β1, mNaV1.6/β1 and, to a lesser extent, hNaV1.5/β1, while the other mammalian isoforms remain unaffected. Importantly, CgNa was also examined on the insect sodium channel DmNaV1/tipE, revealing a clear phyla-selectivity in the efficacious actions of the toxin. CgNa strongly inhibits the inactivation of the insect NaV channel, resulting in a dramatic increase in peak current amplitude and complete removal of fast and steady-state inactivation. Together with the previously determined solution structure, the subtype-selective effects revealed in this study make of CgNa an interesting pharmacological probe to investigate the functional role of specific NaV channel subtypes. Moreover, further structural studies could provide important information on the molecular mechanism of NaV channel inactivation.
topic Selectivity
Sodium channel
Inactivation
toxin
sea anemone
subtype
url http://journal.frontiersin.org/Journal/10.3389/fphar.2010.00133/full
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