摘要
目的:观察吡那地尔(Pin)和硝苯地平(Nif)对内皮素-1(ET-1)缩血管作用的影响并探讨其作用机理。方法:以ET-1在含Ca2+和不含Ca2+K-H液中预收缩离体大鼠主动脉环,比较Pin和Nif累积给药的扩血管效应。结果:在含Ca2+K-H液中,Pin和Nif均可浓度依赖性地对抗ET-11nmol·L-1的缩血管作用,EC50分别为0.50和0.13μmol·L-1。EC95则分别为32和3696μmol·L-1。Pin100μmol·L-1可完全抑制ET-1诱发的血管收缩,相同浓度的Nif仅具部分抑制作用。在无Ca2+K-H液中,Pin1~50μmol·L-1亦可浓度依赖地对抗ET-11nmol·L-1的缩血管作用,其EC50为3.89μmol·L-1,扩血管作用较在含Ca2+K-H液中减弱8倍。同样条件下,Nif未显示相应的作用。结论:ET-1的缩血管作用既与其阻断ATP敏感性钾通道所中介的细胞外钙内流有关又涉及其激动相应受体所介导的细胞内钙释放。Pin和Nif均可对抗ET-1的缩血管作用,Pin的作用机制涉及其阻断电压依赖性钙通道和抑制细胞内钙释放两方面,而Nif的作用仅与其选择性阻断电压依赖性?
AIM: To observe the effects of pinacidil (Pin) and nifedipine (Nif) on endothelin1(ET1)induced vasoconstriction, and to probe their mechanisms. METHODS: Effects of Pin and Nif, administered by cumulative method, on ET1induced vasoconstriction in calcigerous and calciumfree KH solutions were investigated in the isolated rings of rat aorta. RESULTS: In calcigerous KrebsHenseleit(KH) solution, both Pin and Nif antagnize vasoconstriction induced by ET1 at the concentration of 1 nmol·L-1 in a concentrationdependent manner, The EC50 values for dilating aorta ringspreconstricted with ET1 were 005 and 013 μmol·L-1, while the EC95 values were 32 and 3696 μmol·L-1, respectively. Pin rather than Nif at the concentration of 100 μmol·L-1 could inhibit ET1induced vasoconstriction completely. In the calciumfree KH solution, Pin 1 ̄50 μmol·L-1 also antagnized vasoconstriction induced by ET1 at the concentration of 1 nmol·L-1, but Nif showed no action. Moreover, Pins vasodilatory effects in this vehicle were about 8 times less potent than those in calcigerous KH solution. CONCLUSION: The possible mechanisms underlying the vasodilatory effects of pinacidil on isolated aortapreconstricted with ET1 include blocking extracellular Ca2+ influx and depressing intracellular calcium release. In contrast, Nifs effects only involves its blocking extracellular Ca2+ influx without inhibiting the calcium mobilization from the intracellular storage.
出处
《中国药理学通报》
CAS
CSCD
北大核心
1997年第6期502-505,共4页
Chinese Pharmacological Bulletin
基金
国家医药技术创新重大项目
关键词
吡那地尔
硝苯地平
内皮素
药理
缩血管作用
pinacidil
potassium channel activators
nifedipine
calcium channel antagonists
endothelins.
