Benes J, Parada A, Figueiredo A A, Alves P C, Freitas A P, Learmonth D A, Cunha R A, Garrett J, Soares-da-Silva P
Department of Research & Development, BIAL, 4785 S. Mamede do Coronado, Portugal.
J Med Chem. 1999 Jul 15;42(14):2582-7. doi: 10.1021/jm980627g.
A series of esters of the major metabolite of oxcarbazepine (2), 10, 11-dihydro-10-hydroxy-5H-dibenz[b,f]azepine-5-carboxamide, were synthesized and evaluated for their anticonvulsant and brain sodium channel-blocking properties. The compounds were assayed intraperitoneally and per os in rats against seizures induced by maximal electroshock (MES). Neurologic deficit was evaluated by the rotarod test. The enantiomeric acetates (R)-11 and (S)-12 were the most active of the series against MES-induced seizures with oral ED(50) values at t(max) of 10.9 +/- 2.3 and 4.7 +/- 0.9 mg/kg, respectively. After intraperitoneal administration, carbamazepine (1) behaved more potently than 2 and all other new dibenz[b, f]azepine-5-carboxamide derivatives in the MES test; compounds 2 and 12 were equally potent. In the rotarod test, low doses of 1 produced considerable motor impairment, which did not occur with 2, enantiomeric alcohols (S)-6, (R)-7, and racemic alcohol 8, or racemic acetate 10 or (R)-11. The potencies of the racemic and enantiomerically pure alcohols 8, (S)-6, and (R)-7 derived from 2 in the MES and rotarod test were found to be similar between them, and consequently they exhibit similar protective index values. All three forms of the alcohol and their corresponding acetates (pairs 8 & 10, 6 & 12, and 7 & 11) were found to differ in the MES or rotarod tests; the ED(50) value for (S)-6 against MES-induced seizures was nearly 3-fold that for (S)-12. The protective index also differed markedly between all stereoisomers of the alcohol and their corresponding acetates, most pronouncedly for compound (S)-12 which attained the highest value (12.5) among all compounds tested. Blockade of voltage-sensitive sodium channels was studied by investigating [(3)H]batrachotoxinin A 20-alpha-benzoate ([(3)H]BTX) binding. Acetates (R)-11 and (S)-12 were more potent than the standards 1 and 2 at inhibiting the binding of [(3)H]BTX to sodium channels and the influx of (22)Na(+) into rat brain synaptosomes. It is concluded that acetates (R)-11 and (S)-12 are not simple metabolic precursors of alcohols (R)-7 and (S)-6 in rodents but that they possess anticonvulsant and sodium channel-blocking properties in their own right.
合成了奥卡西平(2)的主要代谢产物10,11 - 二氢 - 10 - 羟基 - 5H - 二苯并[b,f]氮杂卓 - 5 - 甲酰胺的一系列酯,并对其抗惊厥和脑钠通道阻断特性进行了评估。通过腹腔注射和口服给药,在大鼠中针对最大电休克(MES)诱导的癫痫发作对这些化合物进行了测定。通过转棒试验评估神经功能缺损。对映体醋酸酯(R)-11和(S)-12是该系列中对MES诱导的癫痫发作最具活性的,口服ED(50)值在t(max)时分别为10.9±2.3和4.7±0.9 mg/kg。腹腔给药后,在MES试验中卡马西平(1)比2以及所有其他新的二苯并[b,f]氮杂卓 - 5 - 甲酰胺衍生物表现出更强的效力;化合物2和12效力相当。在转棒试验中,低剂量的1会产生相当大的运动障碍,而2、对映体醇(S)-6、(R)-7、外消旋醇8、外消旋醋酸酯10或(R)-11则不会。发现源自2的外消旋和对映体纯醇8、(S)-6和(R)-7在MES和转棒试验中的效力彼此相似,因此它们表现出相似的保护指数值。所有三种形式的醇及其相应的醋酸酯(8与10、6与12、7与11)在MES或转棒试验中均存在差异;(S)-6对MES诱导的癫痫发作的ED(50)值几乎是(S)-12的3倍。醇及其相应醋酸酯的所有立体异构体之间的保护指数也有显著差异,对于化合物(S)-12最为明显,其在所有测试化合物中达到最高值(12.5)。通过研究[(3)H]蟾毒素A 20 - α - 苯甲酸酯([(3)H]BTX)结合来研究电压敏感性钠通道的阻断情况。醋酸酯(R)-11和(S)-12在抑制[(3)H]BTX与钠通道的结合以及(22)Na(+)流入大鼠脑突触体方面比标准品1和2更有效。得出的结论是,醋酸酯(R)-11和(S)-12在啮齿动物中不是醇(R)-7和(S)-6的简单代谢前体,而是它们自身就具有抗惊厥和钠通道阻断特性。
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