Lathers C M, Spivey W H, Suter L E, Lerner J P, Tumer N, Levin R M
Life Sci. 1986 Dec 1;39(22):2121-41. doi: 10.1016/0024-3205(86)90364-4.
The effect of timolol (5 mg/kg, p.o., b.i.d. 7 or 14 days) on cardiac beta adrenergic receptor density, the times to arrhythmia (AR) and death (D), heart rate, mean arterial blood pressure, and postganglionic cardiac sympathetic neural discharge after acute coronary occlusion in cats was examined. In the control animals, receptor densities in the left and right atria did not differ, but were lower than the right ventricle. Left ventricle and septum receptor densities were higher, with the left ventricle the highest. The importance of the gradation of beta receptors with increasing density from base to apex appears to be its relation to cardiac contractile function. Occlusion in cats not treated with timolol did not alter the cardiac beta receptor densities. After timolol for 7 or 14 days, no occlusion, receptor density increased in left ventricle and septum although the increase was only significant after 14 days. A comparison of the beta adrenergic receptor densities in cats pretreated with timolol for 7 or 14 days with or without occlusion revealed that, in general, a decrease (p greater than 0.05) occurred for the occlusion group. Timolol decreased heart rate and blood pressure prior to occlusion. The mean times to AR and D were not significantly increased by either dosing regimen of timolol, although the trend was for an increase in the time to D after 7 days of timolol and an increase in the time to AR and D after 14 days of timolol. When compared with data obtained in saline cats, chronic timolol produced minimal changes in postganglionic cardiac sympathetic neural discharge. Timolol given chronically (p.o.) or acutely (5 mg/kg, i.v. given 15 min prior to occlusion) also did not prevent the cardiac sympathetic discharge associated with the development of AR. The time to AR and D in the acutely treated cats was increased but not significantly. Since cardiac sympathetic neural discharge increased as blood pressure fell in the control period but did not increase after occlusion in the timolol treated animals, the combination of timolol and occlusion may have modified neural discharge via an action on the baroreceptor mechanism. That chronic administration of timolol produces an effect not present in cats in which only occlusion was done is supported by the observation that chronic treatment produced an occlusion-induced decrease in beta adrenergic receptor density.(ABSTRACT TRUNCATED AT 400 WORDS)
研究了噻吗洛尔(5毫克/千克,口服,每日两次,共7或14天)对猫急性冠状动脉闭塞后心脏β肾上腺素能受体密度、心律失常(AR)和死亡(D)时间、心率、平均动脉血压以及节后心脏交感神经放电的影响。在对照动物中,左右心房的受体密度无差异,但低于右心室。左心室和室间隔的受体密度较高,其中左心室最高。从心底到心尖β受体密度逐渐增加的重要性似乎与其与心脏收缩功能的关系有关。未用噻吗洛尔治疗的猫闭塞后心脏β受体密度未改变。噻吗洛尔治疗7或14天后,未闭塞时,左心室和室间隔的受体密度增加,不过仅在14天后增加才显著。比较用噻吗洛尔预处理7或14天且有或无闭塞的猫的β肾上腺素能受体密度发现,一般来说,闭塞组出现了降低(p大于0.05)。噻吗洛尔在闭塞前降低心率和血压。噻吗洛尔的两种给药方案均未显著增加AR和D的平均时间,尽管趋势是噻吗洛尔治疗7天后D时间增加,噻吗洛尔治疗14天后AR和D时间增加。与生理盐水处理的猫的数据相比,慢性噻吗洛尔对节后心脏交感神经放电产生的变化极小。慢性(口服)或急性(5毫克/千克,在闭塞前15分钟静脉注射)给予噻吗洛尔也不能预防与AR发生相关的心脏交感神经放电。急性治疗的猫中AR和D的时间增加但不显著。由于在对照期血压下降时心脏交感神经放电增加,而在噻吗洛尔治疗的动物闭塞后未增加,噻吗洛尔与闭塞的联合作用可能通过对压力感受器机制的作用改变了神经放电。慢性给予噻吗洛尔产生仅进行闭塞的猫中不存在的效应,这一观察结果支持了这一点,即慢性治疗导致闭塞引起的β肾上腺素能受体密度降低。(摘要截断于400字)
