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β1-和β2-肾上腺素能受体刺激对大鼠循环镁离子的差异调节

Differential regulation of circulating Mg2+ in the rat by beta 1- and beta 2-adrenergic receptor stimulation.

作者信息

Keenan D, Romani A, Scarpa A

机构信息

Department of Physiology and Biophysics, Case Western Reserve University, School of Medicine, Cleveland, OH 44106, USA.

出版信息

Circ Res. 1995 Nov;77(5):973-83. doi: 10.1161/01.res.77.5.973.

Abstract

Extracellular Mg2+ homeostasis was studied in vivo in the anesthetized rat. Animals were infused with isoproterenol (ISO) for 10 minutes, and serum Mg2+ was measured after the infusion and then 10 and 20 minutes later. A dose-dependent increase in circulating Mg2+ was observed in animals infused with ISO at a rate of 0.1 microgram.kg-1.min-1 or higher. The time course of the effect demonstrated that circulating Mg2+ continued to increase 20 minutes after the end of the ISO infusion. A predicted maximal increase in serum Mg2+ concentration of 19.3% was derived with a predicted EC50 of 0.08 microgram.kg-1.min-1. The maximal percent increase corresponded to a net increase of 6.7 mumol/300 g body wt. Because infusion of ISO resulted in changes in hemodynamic parameters, most notably a drop in blood pressure, a group of animals was infused with nitroprusside to mimic the hypotensive response via a nonadrenergic mechanism. Under these conditions, there was a transient increase in circulating Mg2+ that was largely inhibited by propranolol, indicating that hypotension per se was not responsible for the mobilization of Mg2+. Infusion of salbutamol, but not prenalterol, also induced an increase in circulating Mg2+. Pretreatment with butoxamine, ICI-118551, or propranolol prevented the ISO-induced increase in serum Mg2+. Pretreatment with atenolol minimally affected the ISO-induced changes in circulating Mg2+. Pretreatment with CGP-20271A actually enhanced the ISO-induced increase in circulating Mg2+. This evidence demonstrates the existence of a pool of Mg2+ that is mobilized into the circulation in response to selective beta 2-adrenergic stimulation.

摘要

在麻醉大鼠体内研究了细胞外镁离子(Mg2+)稳态。给动物输注异丙肾上腺素(ISO)10分钟,输注后以及10分钟和20分钟后测量血清Mg2+。以0.1微克·千克-1·分钟-1或更高的速率输注ISO的动物中,观察到循环Mg2+呈剂量依赖性增加。效应的时间进程表明,ISO输注结束后20分钟循环Mg2+仍在继续增加。预测血清Mg2+浓度的最大增加量为19.3%,预测的半数有效浓度(EC50)为0.08微克·千克-1·分钟-1。最大百分比增加对应于净增加6.7微摩尔/300克体重。由于输注ISO导致血液动力学参数发生变化,最明显的是血压下降,因此给一组动物输注硝普钠以通过非肾上腺素能机制模拟低血压反应。在这些条件下,循环Mg2+有短暂增加,而普萘洛尔在很大程度上抑制了这种增加,这表明低血压本身并非Mg2+动员的原因。输注沙丁胺醇而非普瑞特罗也会诱导循环Mg2+增加。用布托沙明、ICI-118551或普萘洛尔预处理可防止ISO诱导的血清Mg2+增加。用阿替洛尔预处理对ISO诱导的循环Mg2+变化影响最小。用CGP-20271A预处理实际上增强了ISO诱导的循环Mg2+增加。这一证据表明存在一组Mg2+,其可响应选择性β2-肾上腺素能刺激而动员到循环中。

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