对人腺苷A3受体具有高选择性的新型N6-取代腺苷5'-N-甲基脲酰胺可减轻缺血性心肌损伤。
Novel N6-substituted adenosine 5'-N-methyluronamides with high selectivity for human adenosine A3 receptors reduce ischemic myocardial injury.
作者信息
Tracey W Ross, Magee William P, Oleynek Joseph J, Hill Roger J, Smith Andrew H, Flynn David M, Knight Delvin R
机构信息
Department of Cardiovascular and Metabolic Diseases, Pfizer Global Research and Development, MS8220-3125, Eastern Point Rd., Groton, CT 06340, USA.
出版信息
Am J Physiol Heart Circ Physiol. 2003 Dec;285(6):H2780-7. doi: 10.1152/ajpheart.00411.2003. Epub 2003 Aug 14.
We recently reported the identification of a novel human adenosine A3 receptor-selective agonist, (2S,3S,4R,5R)-3-amino-5-[6-[5-chloro-2-(3-methylisoxazol-5-ylmethoxy)benzylamino]purin-9-yl]-4-hydroxytetrahydrofuran-2-carboxylic acid methylamide (CP-608,039), with 1,260-fold selectivity for the human A3 versus human A1 receptor (DeNinno et al., J Med Chem 46: 353-355, 2003). However, because the modest (20-fold) rabbit A3 receptor selectivity of CP-608,039 precludes demonstration of A3-mediated cardioprotection in rabbit models, we identified another member of this class, (2S,3S,4R,5R)-3-amino-5-[6-(2,5-dichlorobenzylamino)purin-9-yl]-4-hydroxytetrahydrofuran-2-carboxylic acid methylamide (CP-532,903), which both retained human A3 receptor selectivity (210-fold; human A3/human A1 Ki: 23/4,800 nM) and had improved rabbit A3 receptor selectivity (90-fold; rabbit A3/rabbit A1 Ki: 23/2,000 nM). Infarct size was measured in Langendorff hearts or in vivo after 30 min of regional ischemia and 120 min of reperfusion. Five-minute perfusion with CP-532,903 before ischemia-reperfusion elicited a concentration-dependent reduction in infarct size in isolated hearts (EC50: 0.97 nM; maximum reduction in infarct size: 77%, P < 0.05 vs. control). Furthermore, administration of CP-532,903 (150 nM) at reperfusion also significantly reduced infarct size by 64% (P < 0.05 vs. control), which was not different (P > or = 0.05) from the cardioprotection provided by the same concentration of drug given before ischemia. The selective rabbit A1 receptor antagonist BWA1433 did not affect CP-532,903-dependent cardioprotection. In vivo, CP-532,903 (1 mg/kg) reduced infarct size by 50% in the absence of significant hemodynamic effects (mean arterial pressure, heart rate, rate-pressure product). CP-532,903 and CP-608,039 represent a novel class of human A3 receptor-selective agonists that may prove suitable for investigation of the clinical cardioprotective efficacy of A3 receptor activation.
我们最近报道了一种新型人腺苷A3受体选择性激动剂(2S,3S,4R,5R)-3-氨基-5-[6-[5-氯-2-(3-甲基异恶唑-5-基甲氧基)苄基氨基]嘌呤-9-基]-4-羟基四氢呋喃-2-羧酸甲酰胺(CP-608,039)的鉴定,其对人A3受体与人A1受体的选择性为1260倍(DeNinno等人,《药物化学杂志》46: 353 - 355,2003年)。然而,由于CP-608,039对兔A3受体的选择性适度(20倍),无法在兔模型中证明A3介导的心脏保护作用,我们鉴定了该类别的另一个成员(2S,3S,4R,5R)-3-氨基-5-[6-(2,5-二氯苄基氨基)嘌呤-9-基]-4-羟基四氢呋喃-2-羧酸甲酰胺(CP-532,903),它既保留了对人A3受体的选择性(210倍;人A3/人A1 Ki:23/4800 nM),又提高了对兔A3受体的选择性(90倍;兔A3/兔A1 Ki:23/2000 nM)。在Langendorff心脏或体内进行30分钟局部缺血和120分钟再灌注后测量梗死面积。在缺血-再灌注前用CP-532,903灌注5分钟可引起离体心脏梗死面积浓度依赖性降低(EC50:0.97 nM;梗死面积最大降低率:77%,与对照组相比P < 0.05)。此外,在再灌注时给予CP-532,903(150 nM)也可使梗死面积显著降低64%(与对照组相比P < 0.05),这与缺血前给予相同浓度药物所提供的心脏保护作用无差异(P≥0.05)。选择性兔A1受体拮抗剂BWA1433不影响CP-532,903依赖性心脏保护作用。在体内,CP-532,903(1 mg/kg)在无明显血流动力学效应(平均动脉压、心率、心率-血压乘积)的情况下使梗死面积降低50%。CP-532,903和CP-608,039代表了一类新型人A3受体选择性激动剂,可能适用于研究A3受体激活的临床心脏保护疗效。
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