Gating of cardiac Na+ channels in excised membrane patches after modification by alpha-chymotrypsin.

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Gating of cardiac Na+ channels in excised membrane patches after modification by alpha-chymotrypsin.

C Valenzuela and P B Bennett, Jr

Department of Pharmacology, Vanderbilt University School of Medicine, Nashville, Tennessee 37232.

ABSTRACT

Single cardiac Na+ channels were investigated after intracellularproteolysis to remove the fast inactivation process in an attemptto elucidate the mechanisms of channel gating and the role ofslow inactivation. Na+ channels were studied in inside-out patchesexcised from guinea-pig ventricular myocytes both before andafter very brief exposure (2-4 min) to the endopeptidase, alpha-chymotrypsin.Enzyme exposure times were chosen to maximize removal of fastinactivation and to minimize potential nonspecific damage tothe channel. After proteolysis, the single channel current-voltagerelationship was approximately linear with a slope conductanceof 18 +/- 2.5 pS. Na+ channel reversal potentials measured beforeand after proteolysis by alpha-chymotrypsin were not changed.The unitary current amplitude was not altered after channelmodification suggesting little or no effect on channel conductance.Channel open times were increased after removal of fast inactivationand were voltage-dependent, ranging between 0.7 (-70 mV) and3.2 (-10 mV) ms. Open times increased with membrane potentialreaching a maximum at -10 mV; at more positive membrane potentials,open times decreased again. Fast inactivation appeared to becompletely removed by alpha-chymotrypsin and slow inactivationbecame more apparent suggesting that fast and slow inactivationnormally compete, and that fast inactivation dominates in unmodifiedchannels. This finding is not consistent with a slow inactivatedstate that can only be entered through the fast inactivatedstate, since removal of fast inactivation does not eliminateslow inactivation. The data indicate that cardiac Na+ channelscan enter the slow inactivated state by a pathway that bypassesthe fast inactivated state and that the likelihood of enteringthe slow inactivated state increases after removal of fast inactivation.

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