Aconitum sp. alkaloids: the modulation of voltage-dependent Na+ channels, toxicity and antinociceptive properties

被引:128
作者
Friese, J
Gleitz, J
Gutser, UT
Heubach, JF
Matthiesen, T
Wilffert, B
Selve, N
机构
[1] GRUNENTHAL GMBH,DEPT PHARMACOL,D-52078 AACHEN,GERMANY
[2] GRUNENTHAL GMBH,DEPT TOXICOL,D-52078 AACHEN,GERMANY
[3] PHARMA BIORES,NL-9470 AE ZUIDLAREN,NETHERLANDS
关键词
Aconitum alkaloid; Na+ channel; toxicity; antinociception;
D O I
10.1016/S0014-2999(97)01268-5
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Alkaloids from Aconitum sp., used as analgesics in traditional Chinese medicine, were investigated to elucidate their antinociceptive and toxic properties considering: (1) binding to Na+ channel epitope site 2, (2) alterations in synaptosomal Na+ and Ca2+ concentration ([Na+](i), [Ca2+](i)), (3) arrhythmogenic action of isolated atria, (4) antinociceptive and (5) acute toxic action In mice. The study revealed a high affinity group (K-i 1 mu M) and a low affinity group (K-i 10 mu M) of alkaloids binding to site 2. The compounds of the high affinity group induce an increase in synaptosomal [Na+](i) and [Ca2+](i) (EC50 3 mu M), are antinociceptive (ED50, 25 mu g/kg), provoke tachyarrhythmia and are highly toxic (LD50 70 mu g/kg), whereas low affinity alkaloids reduce [Ca2+](i), induce bradycardia and are less antinociceptive (ED50 20 mg/kg) and less toxic (LD50 30 mg/kg). These results suggest that the alkaloids can be grouped in Na+ channel activating and blocking compounds, but none of the alkaloids seem to be suitable as analgesics because of the low LD50/ED50 values. (C) 1997 Elsevier Science B.V.
引用
收藏
页码:165 / 174
页数:10
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