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  3. Sex and sex hormonal regulation of the atrial inward rectifier potassium current (IK1): insights into potential pro-arrhythmic mechanisms.
 

Sex and sex hormonal regulation of the atrial inward rectifier potassium current (IK1): insights into potential pro-arrhythmic mechanisms.

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BORIS DOI
10.48620/88213
Date of Publication
July 31, 2025
Publication Type
Article
Division/Institute

Institute of Physiolo...

Institut für Physiolo...

Clinic of Cardiology

Contributor
Giammarino, Lucilla
Institute of Physiology
Lluis, Matas
Alerni, Nicolò
Institute of Physiology
Horváth, András
Institute of Physiology
Vashanthakumar, Varjanyorcid-logo
Institute of Physiology
Nimani, Saranda
Clinic of Cardiology
Institute of Physiology
Barbieri, Miriam
Institute of Physiology
Bains, Sahej
Institute of Physiology
Lopez, Ruben
Institute of Physiology
Louradour, Julien
Institute of Physiology
Ördög, Balazs
Institute of Physiology
Hof, Thomas
Institute of Physiology
Maguy, Ange
Institut für Physiologie - Atrial Fibrillation Group
Conte, Giulio
Auricchio, Angelo
Schotten, Ulrich
Odening, Katja E.
Clinic of Cardiology
Institute of Physiology
Subject(s)

600 - Technology::610...

Series
Cardiovascular Research
ISSN or ISBN (if monograph)
1755-3245
0008-6363
Publisher
Oxford University Press
Language
English
Publisher DOI
10.1093/cvr/cvaf074
PubMed ID
40272446
Uncontrolled Keywords

Atrial Fibrillation

IK1

Sex differences

Sex hormones

Description
Aims
Pronounced sex-differences are known in the incidence of atrial fibrillation (AF). In this study, we aimed to investigate the atrial electrophysiological properties that may underlie sex-differences in AF incidence in the younger population, focusing on IK1, a cardiac ion current important for action potential (AP) stability and triggered activity.Methods And Results
We assessed sex-differences in P-wave morphology in 12-lead ECG in healthy young New Zealand White rabbits. Males presented longer P-wave duration and larger P-wave area compared to females. Patch-clamp experiments were performed in isolated rabbit atrial cardiomyocytes (CMs). Male atrial CMs presented higher DAD incidence, amplitude, and area under the curve (AUC) than females, potentially facilitating the presence of atrial triggered activity in males. Male atrial CMs showed a less hyperpolarized resting membrane potential (RMP), a 50% smaller IK1, and a 26% reduction in Kir2.1 protein expression, a pore forming subunit of IK1, than females. Dihydrotestosterone (DHT) effects were investigated acutely and semi-chronically ex vivo. Experiments showed that the sex-difference in IK1 could be mimicked by DHT. In female atrial CMs, acute and semi-chronic (24h) DHT administration reduced IK1. In the presence of a PKC-inhibitor, DHT-mediated IK1 reduction was not observed in atrial female CMs, suggesting it to be PKC-mediated. Chronic DHT-effects were investigated in vivo in female rabbits after hormone-releasing pellet implantation. After two weeks, animals showed a significantly prolonged and larger P-wave, a smaller atrial IK1 and a trend towards an increased DAD amplitude and AUC.Conclusions
Sex impacts on atrial electrophysiology, leading to sex-differences in P-wave morphology, triggered activity, RMP, and IK1. These sex-differences can be mimicked by sex hormone-treatment, suggesting that sex hormones ‒ particularly DHT ‒ play a pivotal role in mediating sex-differences in atrial electrophysiology. Such sex-differences might impact on the propensity to develop AF, particularly in the younger population.
Handle
https://boris-portal.unibe.ch/handle/20.500.12422/210234
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cvaf074.pdftextAdobe PDF1.16 MBpublishedOpen
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