Splice-variant specific effects of a CACNA1H mutation associated with writer’s cramp

Souza, Ivana A.; Gandini, Maria A.; Zamponi, Gerald W.

Splice-variant specific effects of a CACNA1H mutation associated with writer’s cramp

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13041_2021_Article_861.pdf(1.37 MB)

Date

2021-09-20

Authors

Souza, Ivana A.

Gandini, Maria A.

Zamponi, Gerald W.

Abstract

Abstract The CACNA1H gene encodes the α1 subunit of the low voltage-activated Cav3.2 T-type calcium channel, an important regulator of neuronal excitability. Alternative mRNA splicing can generate multiple channel variants with distinct biophysical properties and expression patterns. Two major splice variants, containing or lacking exon 26 (± 26) have been found in different human tissues. In this study, we report splice variant specific effects of a Cav3.2 mutation found in patients with autosomal dominant writer’s cramp, a specific type of focal dystonia. We had previously reported that the R481C missense mutation caused a gain of function effect when expressed in Cav3.2 (+ 26) by accelerating its recovery from inactivation. Here, we show that when the mutation is expressed in the short variant of the channel (− 26), we observe a significant increase in current density when compared to wild-type Cav3.2 (− 26) but the effect on the recovery from inactivation is lost. Our data add to growing evidence that the functional expression of calcium channel mutations depends on which splice variant is being examined.

Citation

Molecular Brain. 2021 Sep 20;14(1):145

URI

http://hdl.handle.net/1880/113967

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