Heptanol blocked peak sodium conductance in canine cardiac Purkinje cells with half block at 1.3 mM, shifting steady-state availability and activation to close off the INa window current.
Heptanol (1.3 mM to 3.0 mM)
Block of peak sodium conductance (INa)
Heptanol blocks sodium current (INa) in nerve, but its effects on cardiac INa have not been well characterized. Block of INa by heptanol was studied in 16 internally perfused voltage-clamped cardiac Purkinje cells at reduced Na+ (45 mM outside, 0 mM inside). Heptanol block of peak sodium conductance was well described by a single-site binding curve with half block at 1.3 mM (20 degrees C) and showed no "use dependence." With 1.5 mM heptanol, block increased slightly by 0.7%/degrees C from 10 degrees C to 27 degrees C. With 3.0 mM heptanol, steady-state availability shifted by 9.4 +/- 1.3 mV (n = 6) in the hyperpolarizing direction, and steady-state activation shifted by 8.3 +/- 2.2 mV (n = 5) in the depolarizing direction, thus closing off the INa "window current." Heptanol also decreased the time to peak and accelerated the decay of INa. Similar results were found with octanol at lower concentrations. These alcohols have important effects on cardiac INa at concentrations used in studies for cellular uncoupling in heart.
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W L Nelson
University of Washington
Jonathan C. Makielski
Electrophysiology
Circulation Research
Abbott (United Kingdom)
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Nelson et al. (Mon,) reported a other. Heptanol was evaluated on Block of peak sodium conductance (INa). Heptanol blocked peak sodium conductance in canine cardiac Purkinje cells with half block at 1.3 mM, shifting steady-state availability and activation to close off the INa window current.
synapsesocial.com/papers/6a0fb2332badbc352afe8fae — DOI: https://doi.org/10.1161/01.res.68.4.977