首页> 美国卫生研究院文献>The Journal of Physiology >Temperature-induced interconversion of alpha-and beta-adrenoceptors in the frog heart.
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Temperature-induced interconversion of alpha-and beta-adrenoceptors in the frog heart.

机译:温度诱导青蛙心脏中的α-和β-肾上腺素能受体相互转换。

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摘要

1. The effect of ambient temperature on the properties of adrenoceptors mediating inotropic responses was assessed in isolated frog hearts on the basis of the effects and tissue uptake of alpha- and beta-adrenoceptor antagonists. 2. At temperatures of 23degree C and above inotropic responses to adrenaline were antagonized by propranolol (0-4-4-0muM), but were unaffected by phentolamine (26-5muM) and were potentiated by phenoxybenzamine (POB) (0-7-29-5muM). Below 17degree C the activity of propranolol was reduced at least tenfold, and the alpha-adrenoceptor antagonists inhibited responses to both adrenaline and isoprenaline, but not those to CaCL2. 3. The responses of hearts exposed to POB at 14degree C and then tested, after thorough washing, at both 14 and 24degree C were similarly inhibited at both temperatures, i.e. the usual beta-adrenoceptor response did not appear at the higher temperature. Conversely, exposure to POB at 24degree C produced only potentiation at both test temperatures. 4. Parallel to the reciprocal changes in their blocking actions, significantly more (14C)propranolol was retained by hearts exposed at high temperatures and significantly more (3H)POB was bound to the myocardium at low temperatures. Changes in binding and in the pharmaco logical effects of both blocking agents occurred entirely within a relatively narrow temperature range (17-22degree C) Parallel to the change from alpha- to beta-adrenoceptor characteristics with increasing temperature, the sensitivity of the hearts to adrenaline increased about tenfold. 5. Phentolamine (26-5muM) effectively protected hearts from block by (3H)POB at 14degree C, unmasked a potentiation of responses to adrenaline equivalent to that produced by POB at 24degree C, and reduced binding of the label to approximately the level found in unprotected hearts exposed at the higher temperature. At 24degree C, phentolamine did not alter the potentiation produced by (3H)POB, and reduced binding only slightly. There was no significant temperature differential in the amount of (3H)POB bound in the presence of phentolamine. 6. The results presented indicate a close functional and, probably, morphological association of alpha- and beta-adrenoceptors in the frog heart. It is suggested that the two classes of adrenoceptors may represent allosterie conformations of the same structure.
机译:1.根据α-和β-肾上腺素受体拮抗剂的作用和组织摄取情况,在离体的青蛙心脏中评估环境温度对介导变力反应的肾上腺素受体特性的影响。 2.在23度以上的温度下,普萘洛尔(0-4-4-0μM)拮抗对肾上腺素的正性反应,但苯妥拉明(26-5μM)不受其影响,苯氧苯甲胺(POB)(0-7- 29-5μM)。低于17℃,普萘洛尔的活性降低至少十倍,并且α-肾上腺素受体拮抗剂抑制对肾上腺素和异丙肾上腺素的反应,但不抑制对CaCL2的反应。 3.在14°C和14°C和24°C彻底清洗后,暴露于POB并随后进行测试的心脏的响应在两种温度下均受到类似的抑制,即在较高温度下未出现通常的β-肾上腺素受体响应。相反,暴露于24°C的POB仅在两个测试温度下均产生增强作用。 4.与其阻断作用的相互变化平行,在高温下暴露的心脏保留了更多的(14C)普萘洛尔,而​​在低温下显着更多的(3H)POB与心肌结合。两种封闭剂的结合和药理作用的变化完全在相对较窄的温度范围内(17-22摄氏度)发生,与温度升高引起的α-肾上腺素受体特性变化(心脏对肾上腺素的敏感性)平行增加了大约十倍。 5.苯妥拉明(26-5μM)在14°C下有效地保护心脏免受(3H)POB的阻滞,掩盖了对肾上腺素的等效于在24°C下由POB产生的应答的反应,并将标记物的结合降低到大约所发现的水平暴露在高温下未受保护的心脏中。在24°C下,酚妥拉明不会改变(3H)POB产生的增效作用,而只会轻微降低结合力。在苯妥拉明的存在下,(3H)POB的结合量没有明显的温差。 6.提出的结果表明青蛙心脏中的α-和β-肾上腺素能受体功能密切相关,并且可能与形态相关。建议两类肾上腺素受体可能代表相同结构的变构构象。

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