天然心房肽对实验性心功能与心肌酶的影响

以天然心房肽灌流豚鼠离体工作心脏,药后１分钟心率开始减慢,左室压及其微分开始升高;５分钟后逐渐恢复,至１０分钟恢复正常。体外培养大鼠心肌细胞,培养液中乳酸脱氢酶含量在药后２小时减少至４８．５±６．８ｕ,为药前的４２．７％（Ｐ＜０．０１）,药后８小时仍明显低于药前水平。为心房肽的新药开发提示了新思路。     

Effects of inotropic agents on isolated guinea pig heart under conditions that modify calcium pools involved in contractile activation

Positive inotropic effects of strophanthidin were compared with those of isoproterenol, BAY K 8644, grayanotoxin, veratridine, and monensin in electrically stimulated left atrial muscle preparations of guinea pig heart under conditions in which the calcium pool, playing a primary role in contractile activation, was altered. In concentrations that caused similar degrees of increase in developed tension under 1 Hz stimulation, grayanotoxin and strophanthidin caused a relatively large increase in potentiated postrest contraction compared with that caused by isoproterenol, whereas the effect of BAY K 8644 on the postrest contraction was the smallest. The effect of high concentrations of grayanotoxin or strophanthidin, however, resembled that of isoproterenol. The sensitivity of the isolated heart muscle to these agents was compared under conditions in which utilization of various calcium pools contributing to contractile activation was suppressed. Mn2+, which reduces contribution of very superficial Ca2+, reduced sensitivity of heart muscle to the positive inotropic effect of isoproterenol and enhanced the inotropic effect of monensin or veratridine. Verapamil, nifedipine, diltiazem, or ryanodine did not have marked effects on the positive inotropic action of Ca2+, monensin, veratridine, or strophanthidin. These results suggest that the positive inotropic actions of veratridine, grayanotoxin, and strophanthidin share a common mechanism and that low concentrations of strophanthidin may increase loading of Ca2+ pool, which plays an important role in potentiated postrest contraction.     

Effects of guinea pig vasoactive intestinal peptide on the isolated perfused guinea pig heart

The pharmacological effects of guinea pig vasoactive intestinal peptide (VIP) were studied in isolated perfused guinea pig hearts. Bolus injections of VIP produced a dose-dependent tachycardia that was not affected by atenolol. A decrease in amplitude of ventricular contractions occurred in response to all doses of VIP. This response was preceded by a small increase in amplitude in 3 of 6 hearts at the highest dose. VIP produced a decrease in perfusion pressure which was prominent after coronary tone was elevated with [Arg8]-vasopressin. The present findings support speculation that VIP may have a role in the regulation of heart rate and coronary blood flow.     

Effects of ouabain and low temperature on the sodium efflux pump in excised corn roots

Ouabain (0.05 millimolar) and low temperature (4 C) both caused the tissue Na⁺ content of excised 5-day-old corn roots to increase, indicating that there is an inhibition of the Na⁺ efflux pump. Na⁺ efflux was measured utilizing three different methods. Each method gave similar results in terms of rate and ouabain sensitivity. With one of these methods, the compartmental efflux method, it was demonstrated that rates for Na⁺ efflux increase as the external Na⁺ concentration is increased; e.g. the efflux rates are 0.529, 1.78, and 3.64 microequivalents per gram fresh weight per hour for external NaCl concentrations of 1, 10, and 30 millimolar, respectively. The data indicate that the Na⁺ efflux pump is located in the plasmalemma of root cells.     

白藜芦醇对哇巴因所致豚鼠乳头状肌迟后去极化及触发活动的效应

研究旨在应用标准玻璃微电极技术,观察白藜芦醇对哇巴因所引起的离体豚鼠乳头状肌迟后去极化(delayed after depolarization,DAD)及触发活动(triggered activity,TA)的效应。结果显示：(1)预先给予白藜芦醇(30、60、120μmol／L)可剂量依赖性地抑制哇巴因所引起的乳头状肌DAD及TA;(2)预先应用L型钙通道开放剂Bay K8644(0．25μmol／L),可取消白藜芦醇的上述效应;(3)预先应用一氧化氮合酶抑制剂L-NAME(1mmol／L),对白藜芦醇的上述效应无影响;(4)单独应用17β-雌二醇(E2,5μmol／1．0或白藜芦醇(30μmol／L)对DAD及TA无明显影响,而联合应用相同剂量的E2和白藜芦醇则对DAD及TA产生明显的抑制效应;(5)预先应用雌激素受体拮抗剂他莫昔芬(10μmol／L)不能取消白藜芦醇对DAD及TA的抑制作用。以上结果表明,白藜芦醇具有抑制乳头状肌DAD及TA的作用,这一效应可能与其抑制钙离子内流有关,但此作用机制中NO和雌激素受体的作用并不显著。白藜芦醇这种抗心律失常作用对于心血管系统具有一定的保护意义。     

植物性雌激素genistein对哇巴因所致豚鼠乳头状肌迟后去极化及触发活动的效应

应用标准玻璃微电极技术,研究了植物性雌激素genistein(GST)对哇巴因所引起的豚鼠乳头状肌迟后去极化（DAD）及触发活动（TA）的效应,结果如下：（1）预先给予是GST（10,50,100umol/L)剂量依赖性地抑制哇巴因（1umol/L)所引起的鼠乳头状肌DAD及TA;（2）预先应用一氧化氮合酶抑制剂L－NAME（1mmol/L),不影响GST（50μmol/L）对DAD及TA的效应;（3）单独应用17β－雌二醇（E2,5μmol/L）或GST（10μmol/L）对DAD及TA无明显影响,而联合应用相同剂量的GST和E2则产生明显儿应,以上结果提示,GST可能通过抑制钙离子内流从而具有抗心律失常作用,这对于心血管系统的保护有一定意义。