Complex interactions between p.His558Arg and linked variants in the sodium voltage-gated channel alpha subunit 5 (Na V 1.5)

Monica Lopes-Marques; Raquel Silva; Catarina Serrano; Verónica Gomes; Ana Cardoso; Maria João Prata; Antonio Amorim; Luisa Azevedo

doi:10.7717/peerj.13913

Complex interactions between p.His558Arg and linked variants in the sodium voltage-gated channel alpha subunit 5 (Na _V 1.5)

PeerJ. 2022 Aug 17:10:e13913. doi: 10.7717/peerj.13913. eCollection 2022.

Authors

Monica Lopes-Marques^{1

2

3}, Raquel Silva⁴, Catarina Serrano^{1

2

3}, Verónica Gomes^{1

3}, Ana Cardoso^{1

2

3}, Maria João Prata^{1

2

3}, Antonio Amorim^{1

2

3}, Luisa Azevedo^{1

2

3}

Affiliations

¹ IPATIMUP-Institute of Molecular Pathology and Immunology, University of Porto, Porto, Portugal.
² Faculty of Sciences, University of Porto, Porto, Portugal.
³ Population Genetics and Evolution, Institute of Innovation and Investigation in Health (i3S), Porto, Portugal.
⁴ Center for Interdisciplinary Research in Health (CIIS), Universidade Católica Portuguesa, Faculdade de Medicina Dentária, Viseu, Portugal.

Abstract

Common genetic polymorphisms may modify the phenotypic outcome when co-occurring with a disease-causing variant, and therefore understanding their modulating role in health and disease is of great importance. The polymorphic p.His558Arg variant of the sodium voltage-gated channel alpha subunit 5 (Na _V 1.5) encoded by the SCN5A gene is a case in point, as several studies have shown it can modify the clinical phenotype in a number of cardiac diseases. To evaluate the genetic backgrounds associated with this modulating effect, we reanalysed previous electrophysiological findings regarding the p.His558Arg variant and further assessed its patterns of genetic diversity in human populations. The Na _V 1.5 p.His558Arg variant was found to be in linkage disequilibrium with six other polymorphic variants that previously were also associated with cardiac traits in GWAS analyses. On account of this, incongruent reports that Arg558 allele can compensate, aggravate or have no effect on Na _V 1.5, likely might have arose due to a role of p.His558Arg depending on the additional linked variants. Altogether, these results indicate a major influence of the epistatic interactions between SCN5A variants, revealing also that phenotypic severity may depend on the polymorphic background associated to each individual genome.

Keywords: Brugada syndrome; Cardiac channel; Cardiac diseases; Epistasis; Genetic background; Genetic modifier; Linkage disequilibrium; SCN5A variants; Sodium voltage-gated channel alpha subunit 5 (NaV1.5).

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Electrophysiological Phenomena*
Humans
NAV1.5 Voltage-Gated Sodium Channel / genetics
Phenotype
Polymorphism, Genetic*
Sodium

Substances

Sodium
NAV1.5 Voltage-Gated Sodium Channel

Grants and funding

This work was supported by FEDER - Fundo Europeu de Desenvolvimento Regional funds through the COMPETE 2020 - Operational Programme for Competitiveness and Internationalization (POCI), Portugal 2020, and by Portuguese funding through FCT - Fundação para a Ciência e a Tecnologia, within the framework of the Project POCI-01–0145-FEDER-007274 to i3S, UIDB/04279/2020 and UIDP/04279/2020 to CIIS, and by FCT research project POCI-01–0145-FEDER-29723. Catarina Serrano holds a FCT PhD fellowship (SFRH/BD/137925/2018). Ana Cardoso holds a FCT PhD fellowship (SFRH/BD/141702/2018). Verónica Gomes is supported by FCT under the program contract provided in Decree-Law no.57/2016 of August 29. Raquel Silva is supported by FCT and UCP under the CEEC institutional funding ref. CEECINST/00137/2018/CP1520/CT0012. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.