Novel non-synonymous mutations in KCNA5 were identified in 2.3% of patients with early-onset lone atrial fibrillation compared to 0% of healthy controls.
Case-Control (n=523)
Are genetic variants in KCNA5 and KCNAB2 associated with early-onset lone atrial fibrillation?
Absolute Event Rate: 2.28% vs 0%
AIMS: Genetic factors may be important in the development of atrial fibrillation (AF) in the young. KCNA5 encodes the potassium channel α-subunit KV1.5, which underlies the voltage-gated atrial-specific potassium current IKur. KCNAB2 encodes KVβ2, a β-subunit of KV1.5, which increases IKur. Three studies have identified loss-of-function mutations in KCNA5 in patients with idiopathic AF. We hypothesized that early-onset lone AF is associated with high prevalence of genetic variants in KCNA5 and KCNAB2. METHODS AND RESULTS: The coding sequences of KCNA5 and KCNAB2 were sequenced in 307 patients with mean age of 33 years at the onset of lone AF, and in 216 healthy controls. We identified six novel non-synonymous mutations E48G, Y155C, A305T (twice), D322H, D469E, and P488S in KCNA5 in seven patients. None were present in controls. We identified a significantly higher frequency of rare deleterious variants in KCNA5 in the patients than in controls. The mutations were analysed with confocal microscopy and whole-cell patch-clamp techniques. The mutant proteins Y155C, D469E, and P488S displayed decreased surface expression and loss-of-function in patch-clamp studies, whereas E48G, A305T, and D322H showed preserved surface expression and gain-of-function for KV1.5. CONCLUSION: This study is the first to present gain-of-function mutations in KCNA5 in patients with early-onset lone AF. We identified three gain-of-function and three loss-of-function mutations. We report a high prevalence of variants in KCNA5 in these patients. This supports the hypothesis that both increased and decreased potassium currents enhance AF susceptibility.
Christophersen et al. (Fri,) conducted a case-control in early-onset lone atrial fibrillation (n=523). Genetic variants in KCNA5 vs. Healthy controls was evaluated on Presence of novel non-synonymous mutations in KCNA5. Novel non-synonymous mutations in KCNA5 were identified in 2.3% of patients with early-onset lone atrial fibrillation compared to 0% of healthy controls.
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