Department of Experimental Cardiology Heart Center, Amsterdam UMC Location University of Amsterdam, Amsterdam, The Netherlands.
Amsterdam Cardiovascular Sciences, Heart failure & Arrhythmias, Amsterdam, The Netherlands.
Clin Genet. 2024 Jul;106(1):37-46. doi: 10.1111/cge.14504. Epub 2024 Feb 29.
Genetic missense variants in TNNI3K, encoding troponin-I interacting kinase, have been associated with dilated cardiomyopathy (DCM) and observed in families with supraventricular tachycardias (SVT). Previously, a family harboring the TNNI3K-c.1615A > G (p.Thr539Ala) variant presented with congenital junctional ectopic tachycardia (CJET), an arrhythmia that arises from the atrioventricular (AV) node and His bundle. However, this was a relatively small four-generational family with limited genetic testing (N = 3). We here describe a multigenerational family with CJET harboring a novel ultra-rare TNNI3K variant: TNNI3K-c.1729C > T (p.Leu577Phe). Of all 18 variant carriers, 13 individuals presented with CJET, resulting in a genetic penetrance of 72%. In addition, CJET is reported in another small family harboring TNNI3K-c.2225C > T (p.Pro742Leu). Similar to the previously published CJET family, both TNNI3K variants demonstrate a substantial reduction of kinase activity. Our study contributes novel evidence supporting the involvement of TNNI3K genetic variants as significant contributors to CJET, shedding light on potential mechanisms underlying this cardiac arrhythmia.
编码肌钙蛋白 I 相互作用激酶的 TNNI3K 中的遗传错义变异与扩张型心肌病 (DCM) 相关,并在伴有室上性心动过速 (SVT) 的家族中观察到。先前,一个携带 TNNI3K-c.1615A>G(p.Thr539Ala) 变异的家族表现为先天性交界性心动过速 (CJET),这是一种起源于房室 (AV) 结和希氏束的心律失常。然而,这是一个相对较小的四代家族,遗传检测有限 (N=3)。我们在这里描述了一个携带 CJET 的多代家族,该家族携带有一个新的超罕见 TNNI3K 变异:TNNI3K-c.1729C>T(p.Leu577Phe)。在所有 18 个变异携带者中,有 13 人出现 CJET,遗传外显率为 72%。此外,另一个携带 TNNI3K-c.2225C>T(p.Pro742Leu) 的小家族也报道了 CJET。与先前发表的 CJET 家族一样,这两种 TNNI3K 变异均显示激酶活性显著降低。我们的研究提供了新的证据,支持 TNNI3K 遗传变异作为 CJET 的重要贡献者,为这种心律失常的潜在机制提供了启示。
