HCN通道在β3-肾上腺素能受体介导的大鼠膀胱舒张中的作用

M. Kashyap, N. Yoshimura, Phillip P Smith, M. Chancellor, P. Tyagi
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引用次数: 13

摘要

目的第二信使cAMP参与β3肾上腺素能受体(β3- ar)介导的逼尿肌舒张和超极化激活环核苷酸门控(HCN)通道动力学。本文研究了HCN通道的激活作用及其与膀胱β3-AR的可能相互作用。材料与方法取Sprague-Dawley大鼠和人器官供体膀胱组织,采用实时荧光定量pcr和Western Blot技术研究HCN通道的种特异性表达。在拉莫三嗪和ZD7288分别激活和阻断HCN通道时,研究β3激动剂对大鼠膀胱条(0.5 × 0.5 × 7 mm)的影响。结果编码HCN通道的4个基因(HCN1-4)分别在人和大鼠膀胱粘膜和逼尿肌中表达。人类膀胱中HCN4亚型和大鼠膀胱中HCN1亚型的表达相对较高,可见物种差异。Western blot在mRNA水平上证实了上述结果。累积应用β3-AR激动剂CL316,243使大鼠膀胱条静息张力以机械活动积分表示,产生浓度依赖性降低。HCN通道阻滞剂zd7288与cl316243的松弛作用相反,而拉莫三嗪与cl316243以等摩尔浓度共给药可引起静息张力的加性降低。累积加入ZD7288和拉莫三嗪对逼尿肌收缩力的影响与不加入cl316243相反。结论膀胱HCN通道的表达存在物种特异性差异。ZD7288和拉莫三嗪在β3-AR激动剂作用中的相反作用表明HCN通道和β3-AR在逼尿肌收缩中可能存在功能相互作用。
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Characterization of the role of HCN channels in β3-adrenoceptor mediated rat bladder relaxation
Objective The second messenger cAMP is involved in both β3 adrenoceptor (β3-AR) mediated detrusor relaxation and the kinetics of Hyperpolarization-activated cyclic nucleotide-gated (HCN) channels. Here we characterized the effect HCN channel activation and possible interaction with β3-AR in bladder. Materials and Methods Bladder tissues from Sprague-Dawley rats and Human organ donors were obtained for studying species-specific expression of HCN channels by real-time qPCR and Western Blot. Effect of β3-agonist on rat bladder strips (0.5 × 0.5 × 7 mm in size) was studied during activation and blockade of HCN channels by Lamotrigine and ZD7288, respectively. Results Expression of all four genes encoding for HCN channels (HCN1-4) was detected separately in bladder mucosa and detrusor from human and rat bladders. Species based differences were evident from relatively higher expression of HCN4 isoform in human bladder and that of HCN1 in rat bladder. Western blot confirmed the findings at mRNA level. Cumulative application β3-AR agonist CL316,243 produced a concentration dependent decrease in resting tension of rat bladder strips expressed as integral of mechanical activity. Pre-incubation of HCN channel blocker ZD 7288 opposed the relaxant effect of CL316,243, whereas co-administration of lamotrigine with CL316,243 at equal molar concentrations caused an additive decrease in resting tension. Cumulative addition of ZD7288 and lamotrigine in absence of CL316,243 showed opposing effects on detrusor contractility. Conclusions Species-specific differences were noted in expression of HCN channels in bladder. Opposing effects ZD7288 and Lamotrigine in the action of β3-AR agonist demonstrate possible functional interaction of HCN channels and β3-AR in detrusor contractility.
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