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• W2300380496 abstract "The blocking effects of cilnidipine and other dihydropyridines on L-type cardiac Ca2+ channels (ICa,L) and N-type sympathetic Ca2+ channel currents (ICa,N) were studied using a whole-cell patch-clamp technique. At −80 mV, cilnidipine had little inhibitory effect below concentrations of 1 μM on ICa,L (IC50 value; 17 μM). However, 1 μM cilnidipine strongly shifted the steady-state inactivation curve of ICa,L toward negative potentials without changing the current–voltage relationship. Each action of cilnidipine was characterized by a high affinity for the inactivated channel in preference to the resting channel. The IC50 values of dihydropyridines for ICa,L were in the range between 0.01 and 10 μM, and those for ICa,N were between 3 and 30 μM. Cilnidipine had the strongest affinity for ICa,N among the dihydropyridines tested. These results suggest that cilnidipine did not cause hypotension-evoked tachycardia deficiency by depression of cardiac L-type channels but by sympathetic N-type channels blockade." @default.
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• W2300380496 date "1999-05-01" @default.
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• W2300380496 title "Selectivity of dihydropyridines for cardiac L-type and sympathetic N-type Ca2+ channels" @default.
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• W2300380496 doi "https://doi.org/10.1016/s0014-2999(99)00237-x" @default.
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