RnoALTD0026735-2/3 @ rn6

In conditions where the intrinsic properties of the Na(V)1.7 splice variants were similar when expressed alone, co-expression of beta1 subunits had different effects on channel availability that were determined by splicing at either site in the alpha subunit. The length of exon 11 regulated how far beta1 subunits depolarised voltage-dependence of inactivation (P_=_0.00012). The results could have a significant impact on channel availability, for example with the long version of exon 11, the co-expression of beta1 subunits could lead to nearly twice as large an increase in channel availability compared to channels containing the short version. These data suggest that splicing can change the way that Na(V) channels interact with beta subunits. Because splicing is conserved, its unexpected role in regulating the functional impact of beta subunits may apply to multiple voltage-gated sodium channels, and the full repertoire of beta subunit function may depend on splicing in alpha subunits.

In conditions where the intrinsic properties of the Na(V)1.7 splice variants were similar when expressed alone, co-expression of beta1 subunits had different effects on channel availability that were determined by splicing at either site in the alpha subunit. The length of exon 11 regulated how far beta1 subunits depolarised voltage-dependence of inactivation (P_=_0.00012). The results could have a significant impact on channel availability, for example with the long version of exon 11, the co-expression of beta1 subunits could lead to nearly twice as large an increase in channel availability compared to channels containing the short version. These data suggest that splicing can change the way that Na(V) channels interact with beta subunits. Because splicing is conserved, its unexpected role in regulating the functional impact of beta subunits may apply to multiple voltage-gated sodium channels, and the full repertoire of beta subunit function may depend on splicing in alpha subunits.