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心脏毒蕈碱受体随年龄增长而减少。体外和体内研究。

Cardiac muscarinic receptors decrease with age. In vitro and in vivo studies.

作者信息

Brodde O E, Konschak U, Becker K, Rüter F, Poller U, Jakubetz J, Radke J, Zerkowski H R

机构信息

Institute of Pharmacology and Toxicology, Martin Luther University Halle-Wittenberg, D-06097 Halle/Saale, Germany.

出版信息

J Clin Invest. 1998 Jan 15;101(2):471-8. doi: 10.1172/JCI1113.

Abstract

The M1 muscarinic receptor antagonist pirenzepine in low doses decreases resting heart rate; this effect declines with age (Poller, U., G. Nedelka, J. Radke, K. Pönicke, and O.-E. Brodde. 1997. J. Am. Coll. Cardiol. 29:187-193). To study possible mechanisms underlying this effect, we assessed (a) in six young (26 yr old) and six older volunteers (61 yr old), pirenzepine effects (0.32 and 0.64 mg intravenous [i.v.] bolus) on isoprenaline-induced heart rate increases; (b) in five heart transplant recipients, pirenzepine effects (0.05-10 mg i.v. bolus) on resting heart rate in the recipient's native and transplanted sinus nodes; and (c) in right atria from 39 patients of different ages (5 d-76 yr) undergoing open heart surgery, M2 muscarinic receptor density (by [3H]N-methyl-scopolamine binding) and adenylyl cyclase activity. (a) Pirenzepine at both doses decreased heart rate in young volunteers significantly more than in older volunteers; (b) pirenzepine (< 1 mg) decreased resting heart rate in the recipient's native but not transplanted sinus node; and (c) M2 receptor density and carbachol-induced inhibition of forskolin-stimulated adenylyl cyclase activity decreased significantly with the age of the patients. We conclude that pirenzepine decreases heart rate via inhibition of presynaptic M1 autoreceptors, thereby releasing endogenous acetylcholine, and that the heart rate-decreasing effect of acetylcholine declines with age because right atrial M2 receptor density and function decrease.

摘要

M1毒蕈碱受体拮抗剂哌仑西平小剂量使用时可降低静息心率;这种作用会随着年龄增长而减弱(Poller, U., G. Nedelka, J. Radke, K. Pönicke, and O.-E. Brodde. 1997. 《美国心脏病学会杂志》29:187 - 193)。为研究该作用潜在的机制,我们评估了:(a) 在6名年轻(26岁)和6名年长志愿者(61岁)中,哌仑西平(静脉推注0.32和0.64 mg)对异丙肾上腺素引起的心率增加的影响;(b) 在5名心脏移植受者中,哌仑西平(静脉推注0.05 - 10 mg)对受者自身及移植窦房结静息心率的影响;以及(c) 在39名不同年龄(5天至76岁)接受心脏直视手术患者的右心房中,M2毒蕈碱受体密度(通过[³H]N - 甲基东莨菪碱结合法)和腺苷酸环化酶活性。(a) 两种剂量的哌仑西平降低年轻志愿者心率的幅度显著大于年长志愿者;(b) 哌仑西平(<1 mg)降低了受者自身窦房结的静息心率,但对移植窦房结无此作用;(c) M2受体密度以及卡巴胆碱对福斯高林刺激的腺苷酸环化酶活性的抑制作用随患者年龄的增加而显著降低。我们得出结论,哌仑西平通过抑制突触前M1自身受体来降低心率,从而释放内源性乙酰胆碱,并且乙酰胆碱降低心率的作用会随着年龄增长而减弱,因为右心房M2受体密度和功能下降。

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