Investigation of CACNA1I Cav3.3 Dysfunction in Hemiplegic Migraine

Maksemous, Neven; Blayney, Claire D.; Sutherland, Heidi G.; Smith, Robert A.; Lea, Rod A.; Tran, Kim Ngan Thi; Ibrahim, Omar; McArthur, Jeffrey R.; Haupt, Larisa M.; Cader, M Z; Finol‐Urdaneta, Rocio K.; Adams, David J.; Griffiths, Lyn R.

doi:10.3389/fnmol.2022.892820

Cited by 9 publications

(4 citation statements)

References 70 publications

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“…Given that the R132H variant implicates the introduction of histidine within the extracellular end of the second transmembrane helix of Ca v 3.2, we assessed the effects of extracellular pH changes, alkalization (pH e 8.0) and acidification (pH e 6.5), on T-type currents. Consistent with previous results on T-type channels [11,12], extracellular alkalization and acidification produced a significant increase and decrease of the T-type current, respectively, in both Ca v 3.2 WT-and R132H-expressing cells (Fig. 1i, top panels).…”

supporting

confidence: 92%

Electrophysiological characterization of a Cav3.2 calcium channel missense variant associated with epilepsy and hearing loss

Stringer,

Cmarko,

Zamponi

et al. 2023

Mol Brain

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T-type calcium channelopathies encompass a group of human disorders either caused or exacerbated by mutations in the genes encoding different T-type calcium channels. Recently, a new heterozygous missense mutation in the CACNA1H gene that encodes the Cav3.2 T-type calcium channel was reported in a patient presenting with epilepsy and hearing loss—apparently the first CACNA1H mutation to be associated with a sensorineural hearing condition. This mutation leads to the substitution of an arginine at position 132 with a histidine (R132H) in the proximal extracellular end of the second transmembrane helix of Cav3.2. In this study, we report the electrophysiological characterization of this new variant using whole-cell patch clamp recordings in tsA-201 cells. Our data reveal minor gating alterations of the channel evidenced by a mild increase of the T-type current density and slower recovery from inactivation, as well as an enhanced sensitivity of the channel to external pH change. To what extend these biophysical changes and pH sensitivity alterations induced by the R132H mutation contribute to the observed pathogenicity remains an open question that will necessitate the analysis of additional CACNA1H variants associated with the same pathologies.

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supporting

confidence: 92%

Electrophysiological characterization of a Cav3.2 calcium channel missense variant associated with epilepsy and hearing loss

Stringer,

Cmarko,

Zamponi

et al. 2023

Mol Brain

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“…Furthermore, CACNA1I and CACNA1H may be implicated in HM [39,125]. Patients with HM have been found to have an increased burden of missense variants in these two genes, further supporting the hypothesis that the genetic architecture of HM extends beyond the currently known genetic area for HM.…”

Section: Other Potential Genes Associated With Fhmmentioning

confidence: 73%

“…Adding to the complexity of understanding the interplay between the human genome and migraine development is the fact that the involvement of mutations in the three known FHM genes is not always established in patients with FHM; this supports the speculation that there might be unknown genes involved in FHM [38]. For example, a recent study found that genetic variants in the CACNA1I gene might contribute to the aetiology of HM [39]. A Danish study on FHM revealed that only 14% of the affected individuals had mutations in the three known genes.…”

Section: Fhm and The Three Known Genesmentioning

confidence: 95%

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Unravelling the Genetic Landscape of Hemiplegic Migraine: Exploring Innovative Strategies and Emerging Approaches

Alfayyadh,

Maksemous,

Sutherland

et al. 2024

Genes

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Migraine is a severe, debilitating neurovascular disorder. Hemiplegic migraine (HM) is a rare and debilitating neurological condition with a strong genetic basis. Sequencing technologies have improved the diagnosis and our understanding of the molecular pathophysiology of HM. Linkage analysis and sequencing studies in HM families have identified pathogenic variants in ion channels and related genes, including CACNA1A, ATP1A2, and SCN1A, that cause HM. However, approximately 75% of HM patients are negative for these mutations, indicating there are other genes involved in disease causation. In this review, we explored our current understanding of the genetics of HM. The evidence presented herein summarises the current knowledge of the genetics of HM, which can be expanded further to explain the remaining heritability of this debilitating condition. Innovative bioinformatics and computational strategies to cover the entire genetic spectrum of HM are also discussed in this review.

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CaV3.3 Channelopathies

Ghaleb

Flucher

2023

Handbook of Experimental Pharmacology

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Investigation of CACNA1I Cav3.3 Dysfunction in Hemiplegic Migraine

Cited by 9 publications

References 70 publications

Electrophysiological characterization of a Cav3.2 calcium channel missense variant associated with epilepsy and hearing loss

Electrophysiological characterization of a Cav3.2 calcium channel missense variant associated with epilepsy and hearing loss

Unravelling the Genetic Landscape of Hemiplegic Migraine: Exploring Innovative Strategies and Emerging Approaches

CaV3.3 Channelopathies

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