首页> 美国卫生研究院文献>British Journal of Pharmacology and Chemotherapy >Positive inotropic effects induced by carbachol in rat atria treated with islet-activating protein (IAP)--association with phosphatidylinositol breakdown.
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Positive inotropic effects induced by carbachol in rat atria treated with islet-activating protein (IAP)--association with phosphatidylinositol breakdown.

机译:卡巴胆碱在胰岛激活蛋白(IAP)处理下对大鼠心房的正性肌力作用-与磷脂酰肌醇分解相关。

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摘要

1. To elucidate the functional consequences of phosphatidyl inositol (PI) breakdown produced by activation of the muscarinic receptor of the atrial muscle, and to clarify the subtypes of the muscarinic receptor involved, the effects of muscarinic agonists and antagonists on mechanical function were studied in atria isolated from rats given intravenous islet-activating protein (IAP; 50 micrograms kg-1 body weight) 48-72 h before the experiments. 2. The negative chronotropic and inotropic actions of carbachol (CCh) were attenuated and positive inotropic effects (62.5 +/- 5.8% above basal level) were observed with 10(-5) -10(-3) M CCh. Oxotremorine did not produce positive inotropic effects even in doses as high as 3 x 10(-4) M High doses of carbachol produced positive chronotropic effects, although the effects were weak. 3. Propranolol (10(-7) M) did not modify the positive inotropic effect of carbachol observed in IAP-treated atria, nor was there any change in the tissue cyclic AMP levels after carbachol. 4. High doses (10(-5)-10(-3) M) of carbachol produced PI breakdown in the absence and presence of IAP. Oxotremorine (3 x 10(-4) M) did not produce PI breakdown. In the presence of oxotremorine, the positive inotropic effects and PI breakdown by carbachol were abolished. 5. The positive inotropic effect of carbachol was readily antagonized by atropine but pirenzepine and gallamine exhibited only weak antagonist effects. 6. These results suggest that a muscarinic agonist such as carbachol can produce a positive inotropic effect in IAP-treated atria, in association with PI breakdown, through activation of a muscarinic receptor which shows some similarity to that previously identified in smooth muscles.
机译:1.为了阐明由于激活心房肌毒蕈碱受体而产生的磷脂酰肌醇(PI)分解的功能后果,并阐明所涉及的毒蕈碱受体的亚型,研究了毒蕈碱激动剂和拮抗剂对机械功能的影响。实验前48-72小时,从给予静脉胰岛激活蛋白(IAP; 50微克kg-1体重)的大鼠中分离出心房。 2.用10(-5)-10(-3)M CCh减弱了卡巴胆碱(CCh)的负变时性和变力作用,并观察到正变力作用(比基础水平高62.5 +/- 5.8%)。 Oxotremorine即使在高达3 x 10(-4)M的剂量下也不会产生正性肌力作用,尽管卡巴胆碱的剂量微弱,但仍能产生正性变时作用。 3.普萘洛尔(10(-7)M)不会改变在IAP治疗的心房中观察到的卡巴胆碱的正性肌力作用,在卡巴胆碱后组织循环AMP水平也没有任何变化。 4.在不存在和存在IAP的情况下,大剂量(10(-5)-10(-3)M)的卡巴胆碱会导致PI分解。 Oxotremorine(3 x 10(-4)M)不会产生PI分解。在oxotremorine的存在下,消除了正性肌力作用和卡巴胆碱对PI的分解作用。 5.卡巴胆碱的正性肌力作用很容易被阿托品所拮抗,但哌仑西平和没食子碱仅表现出微弱的拮抗作用。 6.这些结果表明,毒蕈碱激动剂(如卡巴胆碱)可通过激活毒蕈碱受体而激活,在IAP治疗的心房中产生正性肌力作用,并与PI分解相关,这与先前在平滑肌中发现的相似。

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