A Destructive Interaction Mechanism Accounts for Dominant-Negative Effects of Misfolded Mutants of Voltage-Gated Calcium Channels

doi:10.1523/JNEUROSCI.2844-07.2008

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The Journal of Neuroscience, April 23, 2008, 28(17):4501-4511; doi:10.1523/JNEUROSCI.2844-07.2008

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Neurobiology of Disease
A Destructive Interaction Mechanism Accounts for Dominant-Negative Effects of Misfolded Mutants of Voltage-Gated Calcium Channels
Alexandre Mezghrani,¹^* Arnaud Monteil,¹^* Katrin Watschinger,² Martina J. Sinnegger-Brauns,² Christian Barrère,¹ Emmanuel Bourinet,¹ Joël Nargeot,¹ Jörg Striessnig,² and Philippe Lory¹
¹Centre National de la Recherche Scientifique, Unité Mixte de Recherche 5203, Institut de Génomique Fonctionnelle, Institut National de la Santé et de la Recherche Médicale, Unité 661, and Université Montpellier, 34094 Montpellier, France, and ²Abteilung Pharmakologie und Toxikologie, Institut für Pharmazie und Centrum für Molekulare Biowissenschaften Innsbruck, Universität Innsbruck, A-6020 Innsbruck, Austria
Correspondence should be addressed to either Alexandre Mezghrani or Philippe Lory at the above address. Email: alexandre.mezghrani{at}igf.cnrs.fr or Email: philippe.lory{at}igf.cnrs.fr

Channelopathies are often linked to defective protein foldingand trafficking. Among them, the calcium channelopathy episodicataxia type-2 (EA2) is an autosomal dominant disorder relatedto mutations in the pore-forming Ca_v2.1 subunit of P/Q-typecalcium channels. Although EA2 is linked to loss of Ca_v2.1 channelactivity, the molecular mechanism underlying dominant inheritanceremains unclear. Here, we show that EA2 mutants as well as atruncated form (D_I-II) of the Ca_v3.2 subunit of T-type calciumchannel are misfolded, retained in the endoplasmic reticulum,and subject to proteasomal degradation. Pulse-chase experimentsrevealed that misfolded mutants bind to nascent wild-type Ca_vsubunits and induce their subsequent degradation, thereby abolishingchannel activity. We conclude that this destructive interactionmechanism promoted by Ca_v mutants is likely to occur in EA2and in other inherited dominant channelopathies.

Key words: voltage-gated calcium channel; P/Q-type; T-type; dominant-negative activity; episodic ataxia type 2; misfolding; endoplasmic reticulum; proteasome

Received June 22, 2007; revised Feb. 6, 2008; accepted Feb. 29, 2008.

Correspondence should be addressed to either Alexandre Mezghrani or Philippe Lory at the above address. Email: alexandre.mezghrani{at}igf.cnrs.fr or Email: philippe.lory{at}igf.cnrs.fr

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