The KCNH2-IVS9-28A/G mutation causes aberrant isoform expression and hERG trafficking defect in cardiomyocytes derived from patients affected by Long QT Syndrome type 2

Article ID	Journal	Published Year	Pages	File Type
5604460	International Journal of Cardiology	2017	18 Pages	PDF

Abstract

Our results highlight the key role of the KCNH2 intron 9 branch point in the regulation of KCNH2 isoform expression and hERG channel function, and allow to categorize the IVS9-28A/G mutation as LQT2 class 2 mutation. These findings may result in a more personalized clinical management of IVS9-28A/G mutation carriers.

Keywords

HERG Induced pluripotent stem cells Long QT syndrome Trafficking Cardiomyocytes Splicing

Related Topics

Health Sciences Medicine and Dentistry Cardiology and Cardiovascular Medicine

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The KCNH2-IVS9-28A/G mutation causes aberrant isoform expression and hERG trafficking defect in cardiomyocytes derived from patients affected by Long QT Syndrome type 2

Authors

Manuela Mura, Ashish Mehta, Chrishan J. Ramachandra, Rita Zappatore, Federica Pisano, Maria Chiara Ciuffreda, Vincenzo Barbaccia, Lia Crotti, Peter J. Schwartz, Winston Shim, Massimiliano Gnecchi,