A Novel KCNH2 S981fs Mutation Identified by Whole-Exome Sequencing Is Associated with Type 2 Long QT Syndrome.
Yu-Wen ChengChia-Tung WuChi-Jen ChangYung-Hsin YehGwo-Jyh ChangHsin-Yi TsaiLung-An HsuPublished in: International journal of molecular sciences (2023)
KCNH2 loss-of-function mutations cause long QT syndrome type 2 (LQT2), an inherited cardiac disorder associated with life-threatening ventricular arrhythmia. Through whole-exome sequencing, we discovered a novel AGCGACAC deletion (S981fs) in the hERG gene of an LQT2 patient. Using a heterologous expression system and patch clamping, we found that the mutant K channel had reduced cell surface expression and lower current amplitude compared to the wild type. However, functional expression was restored by lowering temperature and using potassium channel inhibitors or openers (E4031, cisapride, nicorandil). Co-immunoprecipitation experiments confirmed the assembly of mutant proteins with wild-type hERG. Confocal imaging showed decreased hERG distribution on the cell membrane in cells expressing S981fs. Notably, treatment with G418 significantly increased hERG current in wild-type/S981fs heterozygotes. In conclusion, our study identifies a novel hERG mutation leading to impaired Kv11.1 function due to trafficking and nonsense-mediated RNA decay defects. These findings shed light on the mechanisms underlying LQT2 and offer potential therapeutic avenues.
Keyphrases
- wild type
- poor prognosis
- case report
- cell surface
- genome wide
- induced apoptosis
- left ventricular
- heart failure
- binding protein
- high resolution
- long non coding rna
- magnetic resonance imaging
- magnetic resonance
- drug induced
- gene expression
- computed tomography
- transcription factor
- copy number
- catheter ablation
- pi k akt
- endoplasmic reticulum stress