De Luca A, Natuzzi F, Falcone G, Duranti A, Lentini G, Franchini C, Tortorella V, Camerino D C
Dipartimento Farmacobiologico, Facoltà di Farmacia, Bari, Italy.
Naunyn Schmiedebergs Arch Pharmacol. 1997 Dec;356(6):777-87. doi: 10.1007/pl00005118.
To search for potent use-dependent blockers of skeletal muscle sodium channels as potential antimyotonic agents, the actions of newly synthesized chiral analogs of mexiletine and tocainide were tested in vitro on sodium currents of single fibers of frog semitendinosus muscle by vaseline-gap voltage clamp method. The effect of each drug on the maximal peak Na+ transient (I(Na) max) was evaluated as both tonic and use-dependent block by using infrequent depolarizing stimulation and trains of pulses at 2-10 Hz frequency, respectively. The mexiletine analog 3-(2,6-dimethylphenoxy)-2-methylpropanamine (Me2), having an increased distance between the phenyl and the amino groups, was less potent than mexiletine in producing a tonic block but produced a remarkable use-dependent block. In fact, the half-maximal concentration (IC50) for tonic block of S(-)-Me2 was 108 microM vs. 54.5 microM of R(-)-mexiletine, but the IC50 was 6.2 times lowered by the 10 Hz stimulation with respect to the 2.4 fold decrease observed with mexiletine. The R(-)-mexiletine and the S(-)-Me2 were about twofold more potent than the corresponding enantiomers in producing a tonic block, but the stereoselectivity attenuated during use-dependent blockade. The more lipophilic 2-(4-chloro-2-methylphenoxy)-1-phenylethylamine (Me1), presently available as raceme, produced a potent and irreversible tonic block of the sodium currents with an IC50 of 29 microM, but had a less pronounced use-dependent inhibition, with a 1.9 fold decrease of the IC50 at 10 Hz. The R(-) isomer of 2',6'-valinoxylidide (To1), a tocainide derivative with an increased hindrance on the chiral carbon atom, was twofold (IC50 = 209 microM) and tenfold (IC50 = 27.4 microM) more potent than R(-)-tocainide in tonic and use-dependent block, respectively. Tocainide was almost devoid of stereoselectivity, whereas the eudismic ratio of To1 [(IC50 S(+)-To1/IC50 R(-)-To1] was 1.7. As for mexiletine and Me2, the stereoselectivity of To1 was the weaker the higher the frequency of stimulation. The cyclic pyrrolo-imidazolonic tocainide analog To2 produced a small tonic block at 500 microM, and 1 min stimulation at 10 Hz was needed to show up a 50% block of I(Na) max. All the compounds produced a left-shift of the steady-state inactivation curve correlated positively with the extent of use-dependent inhibition, with the exception of the cyclic To2 that acted as an open-channel blocker. The highly use-dependent blockers Me2 and To1 might be promising drugs to solve high frequency discharges of action potentials typical of myotonic muscles. Concomitantly the high potency of Me1 and the open-channel block exerted by To2 can represent important features to get selective blockers for skeletal muscle sodium channels.
为了寻找强效的骨骼肌钠通道使用依赖性阻滞剂作为潜在的抗肌强直药物,采用凡士林间隙电压钳法,在体外对新合成的美西律和妥卡尼的手性类似物作用于青蛙半腱肌单纤维的钠电流进行了测试。通过分别使用不频繁的去极化刺激和2 - 10Hz频率的脉冲串,评估每种药物对最大峰值Na⁺瞬变(I(Na) max)的影响,分别作为强直阻滞和使用依赖性阻滞。美西律类似物3-(2,6 - 二甲基苯氧基)-2 - 甲基丙胺(Me2),其苯基和氨基之间的距离增加,在产生强直阻滞后效性比美西律弱,但产生了显著的使用依赖性阻滞。实际上,S(-)-Me2的强直阻滞半数最大浓度(IC50)为108μM,而R(-)-美西律为54.5μM,但在10Hz刺激下IC50降低了6.2倍,而美西律在同样刺激下降低了2.4倍。R(-)-美西律和S(-)-Me2在产生强直阻滞后效性比相应对映体强约两倍,但在使用依赖性阻滞过程中立体选择性减弱。亲脂性更强的2-(4 - 氯 - 2 - 甲基苯氧基)-1 - 苯乙胺(Me1),目前以外消旋体形式存在,对钠电流产生强效且不可逆的强直阻滞,IC50为29μM,但使用依赖性抑制作用不明显,在10Hz时IC50降低了1.9倍。2',6'-瓦利诺昔胺(To1)的R(-)异构体,一种在手性碳原子上具有增加位阻的妥卡尼衍生物,在强直阻滞和使用依赖性阻滞方面分别比R(-)-妥卡尼强两倍(IC50 = 209μM)和十倍(IC50 = 27.4μM)。妥卡尼几乎没有立体选择性,而To1的优映体比例[(IC50 S(+)-To1/IC50 R(-)-To1]为1.7。与美西律和Me2一样,To1的立体选择性在刺激频率越高时越弱。环状吡咯并咪唑酮类妥卡尼类似物To2在500μM时产生小的强直阻滞,需要在10Hz下刺激1分钟才能使I(Na) max出现50%的阻滞。除了作为开放通道阻滞剂的环状To2外,所有化合物都使稳态失活曲线左移,且与使用依赖性抑制程度呈正相关。高度使用依赖性阻滞剂Me2和To1可能是解决肌强直肌肉典型的高频动作电位发放的有前景的药物。同时,Me1的高效性和To2施加的开放通道阻滞可代表获得骨骼肌钠通道选择性阻滞剂的重要特征。
