Clusters of non-truncating mutations of P/Q type Ca2+ channel subunit Cav2.1 causing episodic ataxia 2

Mantuano, Elide

doi:10.1136/jmg.2003.015396

Cited by 39 publications

(36 citation statements)

References 42 publications

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“…The Ca v 2.1 calcium channel subtype regulates neurotransmission throughout the nervous system, but is predominantly expressed within cerebellar Purkinje cells (Usowicz et al, 1992;Stea et al, 1994;Westenbroek et al, 1995). Not surprisingly, cerebellar dysfunction is the primary feature of EA2 attacks, as patients experience bouts of symptoms such as ataxia, migraine and vertigo, in response to Functional expression studies involving EA2 mutations have firmly established that non-or hypo-conductive α 1 2.1 subunits cause the disorder (Guida et al, 2001;Jen et al, 2001;Jouvenceau et al, 2001;Wappl et al, 2002;Imbrici et al, 2004;Spacey et al, 2004;Imbrici et al, 2005;Wan et al, 2005b;Jeng et al, 2006), which is largely but not exclusively associated with expression of α 1 2.1 truncation mutants (Ophoff et al, 1996;Yue et al, 1998;Battistini et al, 1999;Denier et al, 1999;Jen et al, 1999;Denier et al, 2001;van den Maagdenberg et al, 2002;Wappl et al, 2002;Subramony et al, 2003;Jen et al, 2004;Mantuano et al, 2004;Eunson et al, 2005;Spacey et al, 2005;Wan et al, 2005a;Wan et al, 2005b;Scoggan et al, 2006). However, the molecular mechanisms by which nonfunctional α 1 2.1 pores generate disease in EA2 are still debated.…”

Section: Introductionmentioning

confidence: 99%

Dominant-negative suppression of Cav2.1 currents by α12.1 truncations requires the conserved interaction domain for β subunits

Raike

Kordasiewicz

Thompson

et al. 2007

Molecular and Cellular Neuroscience

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Episodic ataxia type 2 (EA2) is an autosomal dominant disorder arising from CACNA1A mutations, which commonly predict heterozygous expression of Ca v 2.1 calcium channels with truncated α 1 2.1 pore subunits. We hypothesized that α 1 2.1 truncations in EA2 exert dominantnegative effects on the function of wild-type subunits. Wild-type and truncated α 1 2.1 subunits with fluorescent-protein tags were transiently co-expressed in cells stably expressing Ca v auxiliary β subunits, which facilitate α 1 -subunit functional expression through high-affinity interactions with the alpha interaction domain (AID). Co-expression of wild-type subunits with truncations often resulted in severely reduced whole-cell currents compared to expression of wild-type subunits alone. Cellular image analyses revealed that current suppression was not due to reduced wild-type expression levels. Instead, the current suppression depended on truncations terminating distal to the AID. Moreover, only AID-bearing α 1 2.1 proteins co-immunoprecipitated with Ca v β subunits. These results indicate that Ca v β subunits may play a prominent role in EA2 disease pathogenesis.

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Section: Introductionmentioning

confidence: 99%

Dominant-negative suppression of Cav2.1 currents by α12.1 truncations requires the conserved interaction domain for β subunits

Raike

Kordasiewicz

Thompson

et al. 2007

Molecular and Cellular Neuroscience

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“…5 Other groups disagree. 12 However, the unusual clinical phenotype in this family may be due to the location of the mutation in part of the Ca(V)2.1 gene product.…”

Section: Discussionmentioning

confidence: 99%

“…4 The main features are episodes of vertigo or ataxia of variable frequency and duration, a permanent cerebellar deficit of variable severity, and a cerebellar atrophy typically starting from the anterior portion of the vermis. 5 Significant clinical overlap exists between these three disorders. …”

Section: Introductionmentioning

confidence: 99%

Infantile nystagmus and late onset ataxia associated with a CACNA1A mutation in the intracellular loop between s4 and s5 of domain 3

Self

Mercer

Boon

et al. 2009

Eye

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“…12 ). Several missense variants in pore-loop regions have been described in the medical literature so far [12][13][14][15][16][17][18][19][20][21][22][23][24] . Structural changes in pore-loop regions can lead to functional changes disabling activation or inactivation of calcium flux 16 .…”

Section: Discussionmentioning

confidence: 99%

Novel missense variant of CACNA1A gene in a Slovak family with episodic ataxia type 2

Petrovičová¹,

Brozman²,

Kurča³

et al. 2017

Biomed Pap Med Fac Univ Palacky Olomouc Czech Repub

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Clusters of non-truncating mutations of P/Q type Ca2+ channel subunit Cav2.1 causing episodic ataxia 2

Cited by 39 publications

References 42 publications

Dominant-negative suppression of Cav2.1 currents by α12.1 truncations requires the conserved interaction domain for β subunits

Dominant-negative suppression of Cav2.1 currents by α12.1 truncations requires the conserved interaction domain for β subunits

Infantile nystagmus and late onset ataxia associated with a CACNA1A mutation in the intracellular loop between s4 and s5 of domain 3

Novel missense variant of CACNA1A gene in a Slovak family with episodic ataxia type 2

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