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介导人体气道对BRL 35135反应的β-肾上腺素能受体亚型。

Beta-adrenoceptor subtypes mediating the airways response to BRL 35135 in man.

作者信息

Newnham D M, Ingram C G, Mackie A, Lipworth B J

机构信息

Department of Clinical Pharmacology, Ninewells Hospital and Medical School, University of Dundee, Dundee.

出版信息

Br J Clin Pharmacol. 1993 Dec;36(6):567-71. doi: 10.1111/j.1365-2125.1993.tb00416.x.

Abstract

1 The purpose of the study was to assess the bronchorelaxant effects of the beta3-adrenoceptor agonist BRL 35135 in normal human airways. 2 Eight healthy male subjects were studied, having previously demonstrated airways responsiveness to inhaled salbutamol 200 microg, with a group mean (+/- s.e. mean) fall in airways resistance (Raw), from baseline, of 37 +/- 5%. 3 Subjects attended the laboratory on 3 separate days, having fasted and taken placebo (PL) or nadolol 20 mg (N20), 2 h previously. 4 After 30 min rest, baseline measurements of Raw, serum potassium, glucose and free fatty acid were performed before subjects were given single oral doses of BRL 35135 8 mg (BRL) or placebo BRL. Measurements were repeated 60 min after the BRL or placebo BRL were given. 5 There was a significant (P < 0.05) fall in Raw (% change from baseline, as means and 95% CI) with PL/BRL: -32(-18, -46), compared with either PL/PL: -8(5, -21), or N20/BRL: -11(2, -24). There was no significant difference between PL/PL and N20/BRL. 6 A similar pattern to Raw was observed for both of the beta2-mediated metabolic responses which were also antagonised by nadolol. For the potassium response (mmol l(-1)), there was a significant (P < 0.05) difference between PL/BRL: -0.50(-0.31, -0.69), in comparison with either PL/PL: 0.08(-0.11, 0.27) or N20/BRL: 0.09(-0.10, 0.28), but values for PL/PL and N20/BRL were not significantly different. In contrast, with the free fatty acid response (nmol 1(-1)), the increase seen with N20/BRL: 85(1.0, 171.0) was significantly (P < 0.05) different from PL/PL: 3.7(-82.3, 89.8), but was not different from PL/BRL: 132.5(46.5, 218.5). 7 In conclusion, BRL 35135 produced airways, potassium and glucose responses which were antagonised by nadolol, whereas the lipolysis response was not. This suggests that there are not functional beta3-adrenoceptors in human airways.

摘要
  1. 本研究的目的是评估β3-肾上腺素能受体激动剂BRL 35135对正常人气道的支气管舒张作用。2. 对8名健康男性受试者进行了研究,这些受试者先前已证明对吸入200微克沙丁胺醇有气道反应性,气道阻力(Raw)从基线下降的组均值(±标准误均值)为37±5%。3. 受试者在3个不同的日子到实验室,此前2小时禁食并服用安慰剂(PL)或20毫克纳多洛尔(N20)。4. 休息30分钟后,在受试者单次口服8毫克BRL 35135(BRL)或安慰剂BRL之前,进行Raw、血清钾、葡萄糖和游离脂肪酸的基线测量。在给予BRL或安慰剂BRL 60分钟后重复测量。5. 与PL/PL组(-8(5,-21))或N20/BRL组(-11(2,-24))相比,PL/BRL组(-32(-18,-46))的Raw有显著下降(从基线的百分比变化,以均值和95%置信区间表示)(P<0.05)。PL/PL组和N20/BRL组之间无显著差异。6. 对于两种由β2介导的代谢反应,观察到与Raw相似的模式,且纳多洛尔也对其有拮抗作用。对于钾反应(毫摩尔/升),PL/BRL组(-0.50(-0.31,-0.69))与PL/PL组(0.08(-0.11,0.27))或N20/BRL组(0.09(-0.10,0.28))相比有显著差异(P<0.05),但PL/PL组和N20/BRL组的值无显著差异。相比之下,对于游离脂肪酸反应(纳摩尔/升),N20/BRL组(85(1.0,171.0))的升高与PL/PL组(3.7(-82.3,89.8))有显著差异(P<0.05),但与PL/BRL组(132.5(46.5,218.5))无差异。7. 总之,BRL 35135产生的气道、钾和葡萄糖反应可被纳多洛尔拮抗,而脂解反应则不然。这表明人类气道中不存在功能性β3-肾上腺素能受体。

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