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

Mezghrani, Alexandre; Monteil, Arnaud; Watschinger, Katrin; Sinnegger-Brauns, Martina J.; Barrère, Christian; Bourinet, Emmanuel; Nargeot, Joël; Striessnig, Jörg; Lory, Philippe

doi:10.1523/jneurosci.2844-07.2008

Cited by 75 publications

(72 citation statements)

References 52 publications

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“…A dominant negative effect of EA2 mutant Ca V 2.1 α-subunit on normal protein has been demonstrated by double transfection methods for mutations producing PTCs as well [6,[11][12][13][14]. However, the present results on leaner mice and the similar phenotype of cacna1a null, knockout and knockdown mice [20][21][22] would indicate that also a haploinsufficiency mechanism can cause ataxia.…”

Section: Discussioncontrasting

confidence: 60%

“…EA2 is an early onset, autosomal dominant disorder characterised by attacks of vertigo/ataxia, visual disturbance, dysarthria, interictal cerebellar deficit of extremely variable severity, and cerebellar atrophy; epilepsy has occasionally been described [9,10]. A dominant negative effect of the Ca V 2.1 mutated protein affecting the wild type product, rather than a haploinsufficiency, has been hypothesised [6,[11][12][13][14]. Loss of function mutations of the mouse orthologue of the CACNA1A gene cause recessive neurological phenotypes, in tottering (cacna1a tg ; tg), leaner (cacna1a tg-la ; tg-la), rocker (cacna1a rkr ) and rolling Nagoya (cacna1a tg-rol ) mice [15,16].…”

Section: Introductionmentioning

confidence: 99%

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Dramatically different levels of cacna1a gene expression between pre-weaning wild type and leaner mice

Veneziano¹,

Albertosi²,

Pesci³

et al. 2011

Journal of the Neurological Sciences

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Loss of function mutations of the CACNA1A gene, coding for the α1A subunit of P/Q type voltage-gated calcium channel (Ca V 2.1), are responsible for Episodic Ataxia type 2 (EA2), an autosomal dominant disorder. A dominant negative effect of the EA2 mutated protein, rather than a haploinsufficiency mechanism, has been hypothesised both for protein-truncating and missense mutations. We analysed the cacna1a mRNA expression in leaner mice carrying a cacna1a mutation leading to a premature stop codon. The results showed a very low mutant mRNA expression compared to the wild type allele. Although the mutant mRNA slightly increases with age, its low level is likely due to degradation by nonsense mediated decay, a quality control mechanism that selectively degrades mRNA harbouring premature stop codons. These data have implications for EA2 in humans, suggesting a haploinsufficiency mechanism at least for some of the CACNA1A mutations leading to a premature stop codon.

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Section: Discussioncontrasting

confidence: 60%

Section: Introductionmentioning

confidence: 99%

Dramatically different levels of cacna1a gene expression between pre-weaning wild type and leaner mice

Veneziano¹,

Albertosi²,

Pesci³

et al. 2011

Journal of the Neurological Sciences

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“…27 We therefore assessed whether the SCA19 missense mutations (T352P, M373I, and S390N) would also affect the subcellular localization/maturation of Kv4.3. Confocal microscopic analysis of transiently transfected HeLa cells revealed that, unlike wild-type Kv4.3 that was mainly located on the plasma membrane (74.5 6 3.5%; Supplementary Fig 2), all 3 mutant proteins showed almost no or markedly reduced cell surface expression (T352P, 4.9 6 0.6%; M373I, 40.4 6 6.7%; S390N, 5.0 6 2.7%; Supplementary Fig 2), but rather accumulated in perinuclear foci (Fig 3A).…”

Section: Resultsmentioning

confidence: 99%

Mutations in potassium channel kcnd3 cause spinocerebellar ataxia type 19

Duarri

Jezierska

Fokkens

et al. 2012

Annals of Neurology

119

130

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Objective:To identify the causative gene for the neurodegenerative disorder spinocerebellar ataxia type 19 (SCA19) located on chromosomal region 1p21‐q21.Methods:Exome sequencing was used to identify the causal mutation in a large SCA19 family. We then screened 230 ataxia families for mutations located in the same gene (KCND3, also known as Kv4.3) using high‐resolution melting. SCA19 brain autopsy material was evaluated, and in vitro experiments using ectopic expression of wild‐type and mutant Kv4.3 were used to study protein localization, stability, and channel activity by patch‐clamping.Results:We detected a T352P mutation in the third extracellular loop of the voltage‐gated potassium channel KCND3 that cosegregated with the disease phenotype in our original family. We identified 2 more novel missense mutations in the channel pore (M373I) and the S6 transmembrane domain (S390N) in 2 other ataxia families. T352P cerebellar autopsy material showed severe Purkinje cell degeneration, with abnormal intracellular accumulation and reduced protein levels of Kv4.3 in their soma. Ectopic expression of all mutant proteins in HeLa cells revealed retention in the endoplasmic reticulum and enhanced protein instability, in contrast to wild‐type Kv4.3 that was localized on the plasma membrane. The regulatory β subunit Kv channel interacting protein 2 was able to rescue the membrane localization and the stability of 2 of the 3 mutant Kv4.3 complexes. However, this either did not restore the channel function of the membrane‐located mutant Kv4.3 complexes or restored it only partially.Interpretation:KCND3 mutations cause SCA19 by impaired protein maturation and/or reduced channel function. ANN NEUROL 2012;72:870–880

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“…These mutations include missense mutations, splice site mutations, and frame shifts the lead to the truncation of the Ca V 2.1 protein junctions and typically lead loss of channel function (Wappl et al, 2002;Kipfer et al, 2013). In addition, dominant negative effects of mutated channels on normal Ca V 2.1 channels have been reported (Jouvenceau et al, 2001;Jeng et al, 2008;Mezghrani et al, 2008;Page et al, 2010). Consistent with what has been observed with Ca V 2.1 null mice, loss of function of Ca V 2.1 due to a premature truncation of the protein has been shown to give rise to absence seizures in one patient with episodic ataxia (Jouvenceau et al, 2001).…”

Section: Ca V 2 Channel Pathophysiologymentioning

confidence: 99%

The Physiology, Pathology, and Pharmacology of Voltage-Gated Calcium Channels and Their Future Therapeutic Potential

Zamponi¹,

Striessnig²,

Koschak³

et al. 2015

Pharmacol Rev

841

992

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

Cited by 75 publications

References 52 publications

Dramatically different levels of cacna1a gene expression between pre-weaning wild type and leaner mice

Dramatically different levels of cacna1a gene expression between pre-weaning wild type and leaner mice

Mutations in potassium channel kcnd3 cause spinocerebellar ataxia type 19

The Physiology, Pathology, and Pharmacology of Voltage-Gated Calcium Channels and Their Future Therapeutic Potential

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