PLoS ONE (Jan 2012)

Changes in channel trafficking and protein stability caused by LQT2 mutations in the PAS domain of the HERG channel.

  • Carol A Harley,
  • Catarina S H Jesus,
  • Ricardo Carvalho,
  • Rui M M Brito,
  • João H Morais-Cabral

DOI
https://doi.org/10.1371/journal.pone.0032654
Journal volume & issue
Vol. 7, no. 3
p. e32654

Abstract

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Inherited human long-QT2 syndrome (LQTS) results from mutations in the gene encoding the HERG channel. Several LQT2-associated mutations have been mapped to the amino terminal cytoplasmic Per-Arnt-Sim (PAS) domain of the HERG1a channel subunit. Here we have characterized the trafficking properties of some LQT2-associated PAS domain mutants and analyzed rescue of the trafficking mutants by low temperature (27°C) or by the pore blocker drug E4031. We show that the LQT2-associated mutations in the PAS domain of the HERG channel display molecular properties that are distinct from the properties of LQT2-associated mutations in the trans-membrane region. Unlike the latter, many of the tested PAS domain LQT2-associated mutations do not result in trafficking deficiency of the channel. Moreover, the majority of the PAS domain mutations that cause trafficking deficiencies are not rescued by a pore blocking drug. We have also explored the in vitro folding stability properties of isolated mutant PAS domain proteins using a thermal unfolding fluorescence assay and a chemical unfolding assay.