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Title: Basal late sodium current is a significant contributor to the duration of action potential of guinea pig ventricular myocytes.
Author: Song Y, Belardinelli L.
Journal: Physiol Rep; 2017 May; 5(10):e13295. PubMed ID: 28554967.
Abstract:
In cardiac myocytes, an enhancement of late sodium current (I_N_aL) under pathological conditions is known to cause prolongation of action potential duration (APD). This study investigated the contribution of I_N_aL under basal, physiological conditions to the APD Whole-cell I_N_aL and the APD of ventricular myocytes isolated from healthy adult guinea pigs were measured at 36°C. The I_N_aL inhibitor GS967 or TTX was applied to block I_N_aL The amplitude of basal I_N_aL and the APD at 50% repolarization in myocytes stimulated at a frequency of 0.17 Hz were -0.24 ± 0.02 pA/pF and 229 ± 6 msec, respectively. GS967 (0.01-1 μmol/L) concentration dependently reduced the basal I_NaL by 18 ± 3-82 ± 4%. At the same concentrations, GS967 shortened the APD by 9 ± 2 to 25 ± 1%. Similarly, TTX at 0.1-10 μmol/L decreased the basal I_NaL by 13 ± 1-94 ± 1% and APD by 8 ± 1-31 ± 2%. There was a close correlation (R² = 0.958) between the percentage inhibition of I_N_aL and the percentage shortening of APD caused by either GS967 or TTX MTSEA (methanethiosulfonate ethylammonium, 2 mmol/L), a Na_V1.5 channel blocker, reduced the I_NaL by 90 ± 5%, suggesting that the Na_V1.5 channel isoform is the major contributor to the basal I_NaL KN-93 (10 μmol/L) and AIP (2 μmol/L), blockers of CaMKII, moderately reduced the basal I_NaL Thus, this study provides strong evidence that basal endogenous I_NaL is a significant contributor to the APD of cardiac myocytes. In addition, the basal I_NaL of guinea pig ventricular myocytes is mainly generated from Na_V1.5 channel isoform and is regulated by CaMKII.

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