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PDE2 activity differs in right and left rat ventricular myocardium and differentially regulates beta(2) adrenoceptor-mediated effects

机译:PDE2活性在右侧和左大鼠心室心肌中不同,差异调节β(2)肾上腺素受体介导的效果

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摘要

The important regulator of cardiac function, cAMP, is hydrolyzed by different cyclic nucleotide phosphodiesterases (PDEs), whose expression and activity are not uniform throughout the heart. Of these enzymes, PDE2 shapes beta(1) adrenoceptor-dependent cardiac cAMP signaling, both in the right and left ventricular myocardium, but its role in regulating beta(2) adrenoceptor-mediated responses is less well known. Our aim was to investigate possible differences in PDE2 transcription and activity between right (RV) and left (LV) rat ventricular myocardium, as well as its role in regulating beta(2) adrenoceptor effects. The free walls of the RV and the LV were obtained from Sprague-Dawley rat hearts. Relative mRNA for PDE2 (quantified by qPCR) and PDE2 activity (evaluated by a colorimetric procedure and using the PDE2 inhibitor EHNA) were determined in RV and LV. Also, beta(2) adrenoceptor-mediated effects (beta(2)-adrenoceptor agonist salbutamol + beta(1) adrenoceptor antagonist CGP-20712A) on contractility and cAMP concentrations, in the absence or presence of EHNA, were studied in the RV and LV. PDE2 transcript levels were less abundant in RV than in LV and the contribution of PDE2 to the total PDE activity was around 25% lower in the microsomal fraction of the RV compared with the LV. beta(2) adrenoceptor activation increased inotropy and cAMP levels in the LV when measured in the presence of EHNA, but no such effects were observed in the RV, either in the presence or absence of EHNA. These results indicate interventricular differences in PDE2 transcript and activity levels, which may distinctly regulate beta(2) adrenoceptor-mediated contractility and cAMP concentrations in the RV and in the LV of the rat heart.
机译:CAMP的重要调节器由不同的循环核苷酸磷酸二酯酶(PDE)水解,其表达和活性在整个心脏中不均匀。在这些酶中,PDE2形状β(1)肾上腺素受体依赖性心脏阵马信号,无论是在右侧和左心室心肌中,但其在调节β(2)肾上腺素受益介质的反应中的作用较少。我们的目的是探讨PDE2转录和右(RV)和左(LV)大鼠心室心肌的可能差异,以及其在调节β(2)肾上腺素受体效应方面的作用。 RV和LV的自由壁是从Sprague-Dawley大鼠心中获得的。在RV和LV中测定PDE2的相对mRNA和PDE2通过比色程序评估并使用PDE2抑制剂EHNA评估)。此外,在RV和eHNA的不存在或存在下,β(2)肾上腺素依有介导的效果(β(2) - β(2) - β(2) - β(2) - 沙肾上腺素+β(1)肾上腺素受体拮抗剂CGP-20712A)在RV和eHNA的不存在或存在下进行抑制剂浓度LV。在RV的RV中,PDE2转录物水平比LV在LV中的贡献在RV的微粒体馏分中,PDE2与PDE活性的总效率较小约为25%。 β(2)在eHNA存在下测量时,肾上腺素依有性激活在LV中增加了LV的阵营水平,但在RV中没有在eHNA的存在或不存在中观察到这种影响。这些结果表明PDE2转录物和活性水平的间隔差异,其可明显调节β(2)肾上腺素受体介导的收缩性和营养浓度在RV和大鼠心脏的LV中。

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