Variable Clinical Appearance of the Kir2.1 Rare Variants in Russian Patients with Long QT Syndrome

Zaklyazminskaya, Elena; Polyak, Margarita; Shestak, Anna; Sadekova, Mariam; Комолятова, В. Н.; Киселева, И И; Макаров, Л. М.; Podolyak, Dmitriy; Glukhov, Grigory; Zhang, Han; Abramochkin, Denis V.; Sokolova, Olga S.

doi:10.3390/genes13040559

Cited by 2 publications

(2 citation statements)

References 29 publications

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“…Mutation V93I is associated with familial atrial fibrillation and can lead to increased channel activity ( Xia et al, 2005 ). In vitro analysis of channel function revealed a gain-of-function for this variant ( Xia et al, 2005 ; Zaklyazminskaya et al, 2022 ). A study of Russian patients with this variant revealed a surprising phenotype without any signs of ATS1 or mild but evident QTc prolongation ( Zaklyazminskaya et al, 2022 ).…”

Section: Resultsmentioning

confidence: 96%

“…In vitro analysis of channel function revealed a gain-of-function for this variant ( Xia et al, 2005 ; Zaklyazminskaya et al, 2022 ). A study of Russian patients with this variant revealed a surprising phenotype without any signs of ATS1 or mild but evident QTc prolongation ( Zaklyazminskaya et al, 2022 ). Thus, the clinical significance of this variant remains unclear; however, it is classified as a potential proarrhythmogenic risk factor.…”

Section: Resultsmentioning

confidence: 96%

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In silico models of the macromolecular NaV1.5-KIR2.1 complex

Stary-Weinzinger

2024

Front. Physiol.

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In cardiac cells, the expression of the cardiac voltage-gated Na+ channel (NaV1.5) is reciprocally regulated with the inward rectifying K+ channel (KIR2.1). These channels can form macromolecular complexes that pre-assemble early during forward trafficking (transport to the cell membrane). In this study, we present in silico 3D models of NaV1.5-KIR2.1, generated by rigid-body protein-protein docking programs and deep learning-based AlphaFold-Multimer software. Modeling revealed that the two channels could physically interact with each other along the entire transmembrane region. Structural mapping of disease-associated mutations revealed a hotspot at this interface with several trafficking-deficient variants in close proximity. Thus, examining the role of disease-causing variants is important not only in isolated channels but also in the context of macromolecular complexes. These findings may contribute to a better understanding of the life-threatening cardiovascular diseases underlying KIR2.1 and NaV1.5 malfunctions.

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Section: Resultsmentioning

confidence: 96%

Section: Resultsmentioning

confidence: 96%

In silico models of the macromolecular NaV1.5-KIR2.1 complex

Stary-Weinzinger

2024

Front. Physiol.

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The network of cardiac KIR2.1: its function, cellular regulation, electrical signaling, diseases and new drug avenues

Li,

van der Heyden

2024

Naunyn-Schmiedeberg's Arch Pharmacol

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The functioning of the human heart relies on complex electrical and communication systems that coordinate cardiac contractions and sustain rhythmicity. One of the key players contributing to this intricate system is the KIR2.1 potassium ion channel, which is encoded by the KCNJ2 gene. KIR2.1 channels exhibit abundant expression in both ventricular myocytes and Purkinje fibers, exerting an important role in maintaining the balance of intracellular potassium ion levels within the heart. And by stabilizing the resting membrane potential and contributing to action potential repolarization, these channels have an important role in cardiac excitability also. Either gain- or loss-of-function mutations, but also acquired impairments of their function, are implicated in the pathogenesis of diverse types of cardiac arrhythmias. In this review, we aim to elucidate the system functions of KIR2.1 channels related to cellular electrical signaling, communication, and their contributions to cardiovascular disease. Based on this knowledge, we will discuss existing and new pharmacological avenues to modulate their function.

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Variable Clinical Appearance of the Kir2.1 Rare Variants in Russian Patients with Long QT Syndrome

Cited by 2 publications

References 29 publications

In silico models of the macromolecular NaV1.5-KIR2.1 complex

In silico models of the macromolecular NaV1.5-KIR2.1 complex

The network of cardiac KIR2.1: its function, cellular regulation, electrical signaling, diseases and new drug avenues

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