Modeling IK1 current modulation by melatonin and luzindole: a benchmark for patch clamp studies

Whole-cell patch-clamp studies often fail to observe the expected effect of melatonin on the IK1 current in cardiomyocytes, which may be due to cytoplasmic dialysis and the loss of key components of the intracellular signaling system. The aim of this study was to develop a simple theoretical model to estimate the expected effect on the IK1 inward-rectifying potassium current in an experiment with intact melatonin signaling. The modeling was performed using a well-established model of rat cardiomyocyte electrophysiology (Pandit et al., 2001). The maximum conductance of IK1 (gK1) channels was chosen as the target for modulation, consistent with the established mechanism of direct receptor-mediated increase in potassium conductance under the action of melatonin.Realistic modulation values were used for the modeling. The -50% value for the antagonist effect of 1 M luzindole was obtained by direct calculation from our experimental data. The +20% value for the agonist effect (melatonin) was determined by generalizing literature data and reflects the typical expected strength of signaling pathway modulation, rather than being strictly tied to a specific concentration.It was shown that modulation of gK1 in the specified ranges leads to significant changes in IK1 amplitude in the physiologically important range of resting potentials. The developed model serves as a "computational benchmark" for validating experimental protocols, allowing one to distinguish methodological artifacts from a true lack of effect.