Neurocardiac pathologies associated with potassium channelopathies

Author:

Singh Veronica1ORCID,Auerbach David S.1ORCID

Affiliation:

1. Department of Pharmacology SUNY Upstate Medical University Syracuse New York USA

Abstract

AbstractVoltage‐gated potassium channels are expressed throughout the human body and are essential for physiological functions. These include delayed rectifiers, A‐type channels, outward rectifiers, and inward rectifiers. They impact electrical function in the heart (repolarization) and brain (repolarization and stabilization of the resting membrane potential). KCNQx and KCNHx encode Kv7.x and Kv11.x proteins, which form delayed rectifier potassium channels. KCNQx and KCNHx channelopathies are associated with both cardiac and neuronal pathologies. These include electrocardiographic abnormalities, cardiac arrhythmias, sudden cardiac death (SCD), epileptiform discharges, seizures, bipolar disorder, and sudden unexpected death in epilepsy (SUDEP). Due to the ubiquitous expression of KCNQx and KCNHx channels, abnormalities in their function can be particularly harmful, increasing the risk of sudden death. For example, KCNH2 variants have a dual role in both cardiac and neuronal pathologies, whereas KCNQ2 and KCNQ3 variants are associated with severe and refractory epilepsy. Recurrent and uncontrolled seizures lead to secondary abnormalities, which include autonomics, cardiac electrical function, respiratory drive, and neuronal electrical activity. Even with a wide array of anti‐seizure therapies available on the market, one‐third of the more than 70 million people worldwide with epilepsy have uncontrolled seizures (i.e., intractable/drug‐resistant epilepsy), which negatively impact neurodevelopment and quality of life. To capture the current state of the field, this review examines KCNQx and KCNHx expression patterns and electrical function in the brain and heart. In addition, it discusses several KCNQx and KCNHx variants that have been clinically and electrophysiologically characterized. Because these channel variants are associated with multi‐system pathologies, such as epileptogenesis, Kv7 channel modulators provide a potential anti‐seizure therapy, particularly for people with intractable epilepsy. Ultimately an increased understanding of the role of Kv channels throughout the body will fuel the development of innovative, safe, and effective therapies for people at a high risk of sudden death (SCD and SUDEP).

Funder

National Institute of Neurological Disorders and Stroke

Publisher

Wiley

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