AI Article Synopsis
- The cardiac electrical impulse relies on the balance of ionic currents in heart cells, specifically the inwardly rectifying potassium current (I(K1)) and sodium current (I(Na)), which are crucial for maintaining the resting membrane potential and facilitating rapid depolarization during action potentials.
- The interaction between I(K1) and I(Na) influences cell excitability and can lead to abnormal heart rhythms, with significant implications for heart health.
- Using various experimental techniques, researchers found that these ionic currents reciprocally modulate the expression of their respective channel proteins (Kir2.1 and Na(V)1.5) through a complex involving the protein SAP97, which affects how well the heart can maintain its rhythm.
Article Abstract
The cardiac electrical impulse depends on an orchestrated interplay of transmembrane ionic currents in myocardial cells. Two critical ionic current mechanisms are the inwardly rectifying potassium current (I(K1)), which is important for maintenance of the cell resting membrane potential, and the sodium current (I(Na)), which provides a rapid depolarizing current during the upstroke of the action potential. By controlling the resting membrane potential, I(K1) modifies sodium channel availability and therefore, cell excitability, action potential duration, and velocity of impulse propagation. Additionally, I(K1)-I(Na) interactions are key determinants of electrical rotor frequency responsible for abnormal, often lethal, cardiac reentrant activity. Here, we have used a multidisciplinary approach based on molecular and biochemical techniques, acute gene transfer or silencing, and electrophysiology to show that I(K1)-I(Na) interactions involve a reciprocal modulation of expression of their respective channel proteins (Kir2.1 and Na(V)1.5) within a macromolecular complex. Thus, an increase in functional expression of one channel reciprocally modulates the other to enhance cardiac excitability. The modulation is model-independent; it is demonstrable in myocytes isolated from mouse and rat hearts and with transgenic and adenoviral-mediated overexpression/silencing. We also show that the post synaptic density, discs large, and zonula occludens-1 (PDZ) domain protein SAP97 is a component of this macromolecular complex. We show that the interplay between Na(v)1.5 and Kir2.1 has electrophysiological consequences on the myocardium and that SAP97 may affect the integrity of this complex or the nature of Na(v)1.5-Kir2.1 interactions. The reciprocal modulation between Na(v)1.5 and Kir2.1 and the respective ionic currents should be important in the ability of the heart to undergo self-sustaining cardiac rhythm disturbances.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3412015 | PMC |
| http://dx.doi.org/10.1073/pnas.1109370109 | DOI Listing |
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