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组胺受体对人体左心室基础收缩张力的影响:使用H2受体拮抗剂法莫替丁和β-肾上腺素能受体拮抗剂艾司洛尔作为药理学探针进行评估。

Influence of histamine receptors on basal left ventricular contractile tone in humans: assessment using the H2 receptor antagonist famotidine and the beta-adrenoceptor antagonist esmolol as pharmacologic probes.

作者信息

Borow K M, Ehler D, Berlin R, Neumann A

机构信息

Department of Medicine, University of Chicago Medical Center, Illinois 60637.

出版信息

J Am Coll Cardiol. 1992 May;19(6):1229-36. doi: 10.1016/0735-1097(92)90329-l.

Abstract

Histamine has a positive inotropic action in humans. Recent controversial data have suggested that histamine2 (H2) receptor blockade depresses overall left ventricular systolic performance in healthy volunteers. To explore the possibility that H2 receptors positively influence basal left ventricular contractile tone, 10 normal subjects were studied by using imaging and Doppler echocardiography and calibrated subclavian pulse data in a blinded, randomized, two-period crossover trial with measurements obtained at the end of each 7-day period. Oral drug administration consisted of either the potent H2 antagonist famotidine (40 mg/day) or placebo. Left ventricular circumferential end-systolic wall stress-rate-corrected velocity of fiber shortening (Vcfc) relations were generated over a range of loads with methoxamine. Contractility was assessed by using Vcfc at a common end-systolic wall stress. During each study, data were obtained before and during high dose intravenous esmolol administration to determine the contributions, if any, of sympathetic reflex responses. Famotidine did not alter blood pressure, left ventricular percent fractional shortening, circumferential end-systolic wall stress, stroke volume index, cardiac index, total vascular resistance or ventricular contractile state in comparison with placebo but did decrease heart rate by 3 beats/min (p less than 0.05). With beta-adrenergic blockade, no differences in contractility were evident between esmolol alone and famotidine plus esmolol. Thus, H2 receptor blockade with famotidine does not alter myocardial mechanics or cardiac sympathetic tone, suggesting that in humans basal left ventricular contractile state is not physiologically dependent on the H2-mediated effects of histamine.

摘要

组胺对人体有正性肌力作用。最近有争议的数据表明,组胺2(H2)受体阻断会降低健康志愿者的整体左心室收缩功能。为了探究H2受体是否对基础左心室收缩张力有正向影响,在一项双盲、随机、两阶段交叉试验中,对10名正常受试者进行了研究,使用成像和多普勒超声心动图以及校准的锁骨下脉搏数据,在每个7天周期结束时进行测量。口服药物为强效H2拮抗剂法莫替丁(40毫克/天)或安慰剂。用甲氧明在一系列负荷下生成左心室圆周收缩末期壁应力-纤维缩短速率校正速度(Vcfc)关系。通过在共同的收缩末期壁应力下使用Vcfc来评估收缩性。在每项研究中,在高剂量静脉注射艾司洛尔之前和期间获取数据,以确定交感反射反应(如有)的贡献。与安慰剂相比,法莫替丁并未改变血压、左心室缩短分数百分比、圆周收缩末期壁应力、每搏量指数、心脏指数、总血管阻力或心室收缩状态,但确实使心率降低了3次/分钟(p<0.05)。在β肾上腺素能阻断的情况下,单独使用艾司洛尔与法莫替丁加艾司洛尔之间在收缩性方面没有明显差异。因此,用法莫替丁阻断H2受体不会改变心肌力学或心脏交感神经张力,表示在人类中基础左心室收缩状态在生理上不依赖于组胺的H2介导作用。

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