Arrhythmia-associated Calmodulin Variants Interact with KCNQ1 to Confer Aberrant Membrane Trafficking and Function.
Po Wei KangLucy WoodburyPaweorn AngsutararuxNamit SambareJingyi ShiMartina MarrasCarlota AbellaAnish BediDeShawn ZinnJianmin CuiJonathan R SilvaPublished in: bioRxiv : the preprint server for biology (2023)
This study provides comprehensive functional data that reveal how CaM variants contribute to creating a pro-arrhythmic substrate by causing abnormal KCNQ1 membrane trafficking and current conduction. We find that CaM variant regulation of KCNQ1 is not uniform with effects varying from benign to significant loss of function. This study provides a new approach to collecting details of CaM binding that are key for understanding how CaM variants predispose patients to arrhythmia via the dysregulation of multiple cardiac ion channels.