Novel Variant in the
            <i>ANK2</i>
            Membrane-Binding Domain Is Associated With Ankyrin-B Syndrome and Structural Heart Disease in a First Nations Population With a High Rate of Long QT Syndrome

Swayne, Leigh Anne; Murphy, Nathaniel P.; Asuri, Sirisha; Chen, Lena; Xu, Xiaoxue; McIntosh, Sarah; Wang, Chao; Lancione, Peter J.; Roberts, Jason D.; Kerr, Charles R.; Sanatani, Shubhayan; Sherwin, Elizabeth D.; Kline, Crystal F.; Zhang, Mingjie; Mohler, Peter J.; Arbour, Laura

doi:10.1161/circgenetics.116.001537

Cited by 37 publications

(51 citation statements)

References 47 publications

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“…The loss-of-function variant was found to prohibit normal membrane targeting of NCX, presumably due to the altered localization of AnkB p.S646F. 38 Ichikawa et al also recently found possibly damaging variants in the MBD in isolated cases of arrhythmia. All other reported disease causing loss-of-function variants occur in the SBD, DD, or C-terminal domain.…”

Section: Human Ank2 Variantsmentioning

confidence: 99%

“…Normal localization of NCX and AnkB was also found to be disrupted in the MBD variant p.S646F, indicating that NCX localization is regulated by two AnkB domains – MBD and RD. 38 ANK2 variants have also been found to cause sinus node disease (SND), and AnkB heterozygous (AnkB +/− ) mice phenocopy human SND patients, presumably due to loss of AnkB-mediated organization and signaling in sinoatrial node (SAN) cells. 34 Another variant in ANK2 that disrupts the AnkB/βII-spectrin interaction (AnkB p.R990Q) causes severe arrhythmia phenotypes.…”

Section: Human Ank2 Variantsmentioning

confidence: 99%

“…65 Furthermore, seizures have been shown to correlate with AnkB-associated cardiac channelopathies. 38, 66, 67 Initially discovered in 1993 and 1995, the 440kDa AnkB (AnkB-440) and 480kDa AnkG (AnkG-480) isoforms, also known as giant ankyrins, are a result of the addition of a single large exon. 68, 69 The role of giant ankyrins in patterning the axon initial segment was demonstrated in Drosophila and was shown to be conserved across Bilatera.…”

Section: Future Investigationsmentioning

confidence: 99%

“…While this finding is significant in itself, this group also reported the presence of congenital malformations associated with the AnkB p.S646F variant. 38 Interestingly, AnkB −/− mice suffer neonatal lethality 21 , which could be associated with a congenital heart defect. Additionally, these families displayed an incidence of cerebral aneurysms, suggesting a novel vascular role for AnkB.…”

Section: Future Investigationsmentioning

confidence: 99%

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The evolving role of ankyrin-B in cardiovascular disease

Koenig

Mohler

2017

Heart Rhythm

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Over the last decade, ankyrin-B has been identified as a prominent player in cardiac physiology. Ankyrin-B has a multitude of functions, with roles in expression, localization, and regulation of proteins critical for cardiac excitability, cytoskeletal integrity, and signaling. Further, human ANK2 variants that result in ankyrin-B loss-of-function are associated with ‘Ankyrin-B syndrome’, a complex cardiac phenotype that may include bradycardia and heart rate variability, conduction block, atrial fibrillation, QT interval prolongation, and potentially fatal catecholaminergic polymorphic ventricular tachycardia. However, our understanding of the molecular mechanisms underlying ankyrin-B function at baseline and in disease is still not fully resolved due to the complexity of ankyrin-B gene regulation, number of ankyrin-B-associated molecules, multiple roles of ankyrin-B in the heart and other organs that modulate cardiac function, and a host of unexpected clinical phenotypes. Here, we summarize known roles of ankyrin-B in the heart and the impact of ankyrin-B dysfunction in animal models and in human disease, as well as highlight important new findings illustrating the complexity of ankyrin-B signaling.

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Section: Human Ank2 Variantsmentioning

confidence: 99%

Section: Human Ank2 Variantsmentioning

confidence: 99%

Section: Future Investigationsmentioning

confidence: 99%

Section: Future Investigationsmentioning

confidence: 99%

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The evolving role of ankyrin-B in cardiovascular disease

Koenig

Mohler

2017

Heart Rhythm

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“…The subsequent association of either Sptbn1 (275 kDa), or Itpr1 (310 kDa) would shift the mass to around 800 kDa. Both Sptan1 and Ank2 have a variety of binding domains where interactions with Kcc2 could occur, such as SH3 domains (Sptan1) (61) and the membrane binding domain containing the Ank repeat sequences of Ank2 (62), which has been shown to interact with other ion channels/transporters (63).…”

Section: Kcc2 Forms Stable Multi-protein Complexes In the Plasma Membmentioning

confidence: 99%

Isolation and characterization of multi-protein complexes enriched in the K-Cl co-transporter 2 from brain plasma membranes

Smalley

Kontou

Choi

et al. 2020

Preprint

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Kcc2 plays a critical role in determining the efficacy of synaptic inhibition, however, the cellular mechanism neurons use to regulate its membrane trafficking, stability and activity are ill-defined. To address these issues, we used affinity purification to isolate stable multi-protein complexes of Kcc2 from the plasma membrane of murine forebrain. We resolved these using Blue-native polyacrylamide gel electrophoresis (BN-PAGE) coupled to LC-MS/MS. Purified Kcc2 migrated as distinct molecular species of 300, 600 and 800 kDa following BN-PAGE. In excess of 90% coverage of the soluble N and C-termini of Kcc2 was obtained. The 300kDa species largely contained Kcc2, which is consistent with a dimeric quaternary structure for this transporter. Intriguingly, lower levels of Kcc1 were also found in this species suggesting the existence of “mixed” Kcc2/Kcc1 heterodimers. The 600 and 800 kDa species represented stable multi-protein complexes of Kcc2. We identified a set of novel structural, ion transporting and signaling protein interactors, that are present at both excitatory and inhibitory synapses, consistent with the proposed association of Kcc2. These included spectrins, ankyrins, and the IP3 receptor. We also identified interactors more directly associated with phosphorylation; Akap5 and Lmtk3. Finally, we used LC-MS/MS on highly purified endogenous plasma membrane Kcc2 to detect phosphorylation sites. We detected 11 sites with high confidence, including known and novel sites. Collectively our experiments demonstrate that Kcc2 is associated with components of the neuronal cytoskeleton and signaling molecules that may act to regulate transporter membrane trafficking, stability, and activity.

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Wolff–Parkinson–White syndrome: De novo variants and evidence for mutational burden in genes associated with atrial fibrillation

Coban‐Akdemir

Charng

Azamian

et al. 2020

American J of Med Genetics Pt A

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Background: Wolff-Parkinson-White (WPW) syndrome is a relatively common arrhythmia affecting~1-3/1,000 individuals. Mutations in PRKAG2 have been described in rare patients in association with cardiomyopathy. However, the genetic basis of WPW in individuals with a structurally normal heart remains poorly understood. Sudden death due to atrial fibrillation (AF) can also occur in these individuals.Several studies have indicated that despite ablation of an accessory pathway, the risk of AF remains high in patients compared to general population. Methods:We applied exome sequencing in 305 subjects, including 65 trios, 80 singletons, and 6 multiple affected families. We used de novo analysis, candidate gene approach, and burden testing to explore the genetic contributions to WPW.Results: A heterozygous deleterious variant in PRKAG2 was identified in one subject, accounting for 0.6% (1/151) of the genetic basis of WPW in this study. Another individual with WPW and left ventricular hypertrophy carried a known pathogenic variant in MYH7. We found rare de novo variants in genes associated with arrhythmia and cardiomyopathy (ANK2, NEBL, PITX2, and PRDM16) in this cohort. There was an increased burden of rare deleterious variants (MAF ≤ 0.005) with CADD score ≥ 25 in genes linked to AF in cases compared to controls (P = .0023).Conclusions: Our findings show an increased burden of rare deleterious variants in genes linked to AF in WPW syndrome, suggesting that genetic factors that determine the development of accessory pathways may be linked to an increased susceptibility of atrial muscle to AF in a subset of patients. K E Y W O R D SANK2, atrial fibrillation, exome sequencing, Wolff-Parkinson-White (WPW) syndrome

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Novel Variant in the ANK2 Membrane-Binding Domain Is Associated With Ankyrin-B Syndrome and Structural Heart Disease in a First Nations Population With a High Rate of Long QT Syndrome

Cited by 37 publications

References 47 publications

The evolving role of ankyrin-B in cardiovascular disease

The evolving role of ankyrin-B in cardiovascular disease

Isolation and characterization of multi-protein complexes enriched in the K-Cl co-transporter 2 from brain plasma membranes

Wolff–Parkinson–White syndrome: De novo variants and evidence for mutational burden in genes associated with atrial fibrillation

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