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Vol. 290, Issue 2, 515-523, August 1999
Unidad de Investigacion "Carlos Mendez," Centro de
Investigaciones Biomedicas de la Universidad de Colima, Colima, Mexico
The block of the transient outward K+ current
(Ito) by disopyramide was studied in isolated rat right
ventricular myocytes using whole cell patch-clamp techniques.
Disopyramide at a concentration of 10 to 1000 µM reduced peak
Ito and accelerated the apparent rate of current
inactivation. The onset of block was assessed using a double pulse
protocol with steps from
70 to +50 mV. As the duration of the first
(conditioning) pulse was increased from 1 to 50 ms, block was
increased. Further prolongation of the conditioning pulse resulted in
relief of block, which was nearly complete with a 1-s conditioning
pulse. In the absence of drug, the recovery from inactivation of
Ito at
70 mV was fast and best fit with a single
exponential function having a time constant of 33 ± 13 ms. In
contrast, in the presence of 100 µM disopyramide, recovery from
apparent inactivation was biexponential with time constants of 35 ± 13 ms and 7.16 ± 1.5 s. The time course of the slow
component was used to estimate recovery of channels from block by
disopyramide. Recovery from block was voltage-dependent, suggesting
that disopyramide was trapped by the open channel. Taken together,
these results suggest that disopyramide rapidly blocks channels in the
open state and that unblock occurs from the inactivated state.
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