Propping Stefan, Lorenz Kristina, Michel Martin C, Wirth Manfred P, Ravens Ursula
Department of Urology, Faculty of Medicine Carl Gustav Carus, Dresden University of TechnologyDresden, Germany; Department of Physiology, Faculty of Medicine Carl Gustav Carus, Dresden University of TechnologyDresden, Germany.
Department of Pharmacology and Toxicology, Julius Maximilian University WürzburgWürzburg, Germany; Leibniz-Institute für Analytische Wissenschaften-ISAS-e.V.Dortmund, Germany; West German Heart and Vascular Center Essen, University Hospital Essen-DuisburgDuisburg, Germany.
Front Pharmacol. 2016 May 9;7:118. doi: 10.3389/fphar.2016.00118. eCollection 2016.
In order to characterize the β-adrenoceptor (AR) subtypes involved in agonist-stimulated relaxation of murine urinary bladder we studied the effects of (-)-isoprenaline and CL 316,243 on tonic contraction and spontaneous contractions in detrusor strips of wild-type (WT) and β2-AR knockout (β2-AR KO) mice.
Urinary bladders were isolated from male WT and β2-AR KO mice. β-AR subtype expression was determined with quantitative real-time PCR. Intact muscle strips pre-contracted with KCl (40 mM) were exposed to cumulatively increasing concentrations of (-)-isoprenaline or β3-AR agonist CL 316,243 in the presence and absence of the subtype-selective β-AR blockers CGP 20712A (β1-ARs), ICI 118,551 (β2-ARs), and L748,337 (β3-ARs).
Quantitative real-time PCR confirmed lack of β2-AR expression in bladder tissue from β2-AR KO mice. In isolated detrusor strips, pre-contraction with KCl increased basal tone and enhanced spontaneous activity significantly more in β2-AR KO than in WT. (-)-Isoprenaline relaxed tonic tension and attenuated spontaneous activity with similar potency, but the concentrations required were two orders of magnitude higher in β2-AR KO than WT. The concentration-response curves (CRCs) for relaxation were not affected by CGP 20712A (300 nM), but were shifted to the right by ICI 118,551 (50 nM) and L748,337 (10 μM). The -logEC50 values for (-)-isoprenaline in WT and β2-AR KO tissue were 7.98 and 6.00, respectively, suggesting a large receptor reserve of β2-AR. (-)-CL 316,243 relaxed detrusor and attenuated spontaneous contractions from WT and β2-AR KO mice with a potency corresponding to the drug's affinity for β3-AR. L743,337 shifted the CRCs to the right.
Our findings in β2-AR KO mice suggest that there is a large receptor reserve for β2-AR in WT mice so that this β-AR subtype will mediate relaxation of tone and attenuation of spontaneous activity under physiological conditions. Nevertheless, upon removal of this reserve, β3-AR can also mediate murine detrusor relaxation.
为了明确参与激动剂刺激的小鼠膀胱舒张的β-肾上腺素能受体(AR)亚型,我们研究了(-)-异丙肾上腺素和CL 316,243对野生型(WT)和β2-AR基因敲除(β2-AR KO)小鼠逼尿肌条中张力收缩和自发收缩的影响。
从雄性WT和β2-AR KO小鼠分离膀胱。用定量实时PCR测定β-AR亚型表达。在存在和不存在亚型选择性β-AR阻滞剂CGP 20712A(β1-ARs)、ICI 118,551(β2-ARs)和L748,337(β3-ARs)的情况下,将预先用氯化钾(40 mM)预收缩的完整肌条暴露于累积增加浓度的(-)-异丙肾上腺素或β3-AR激动剂CL 316,243。
定量实时PCR证实β2-AR KO小鼠膀胱组织中缺乏β2-AR表达。在分离的逼尿肌条中,用氯化钾预收缩后,β2-AR KO小鼠的基础张力增加且自发活动增强的程度明显高于WT小鼠。(-)-异丙肾上腺素以相似的效力舒张张力并减弱自发活动,但β2-AR KO小鼠所需的浓度比WT小鼠高两个数量级。舒张的浓度-反应曲线(CRCs)不受CGP 20712A(300 nM)影响,但ICI 118,551(50 nM)和L748,337(10 μM)使其右移。WT和β2-AR KO组织中(-)-异丙肾上腺素的-logEC50值分别为7.98和6.00,表明β2-AR有大量受体储备。(-)-CL 316,243舒张逼尿肌并减弱WT和β2-AR KO小鼠的自发收缩,其效力与该药物对β3-AR的亲和力相当。L743,337使CRCs右移。
我们在β2-AR KO小鼠中的研究结果表明,WT小鼠中β2-AR有大量受体储备,因此在生理条件下该β-AR亚型将介导张力舒张和自发活动减弱。然而,去除这一储备后,β3-AR也可介导小鼠逼尿肌舒张。
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