β-肾上腺素能受体亚型对成年大鼠心室肌细胞凋亡的影响存在差异。
Beta-adrenergic receptor subtypes differentially affect apoptosis in adult rat ventricular myocytes.
作者信息
Zaugg M, Xu W, Lucchinetti E, Shafiq S A, Jamali N Z, Siddiqui M A
机构信息
Department of Anesthesiology, Health Science Center at Brooklyn, State University of New York, USA.
出版信息
Circulation. 2000 Jul 18;102(3):344-50. doi: 10.1161/01.cir.102.3.344.
BACKGROUND-Catecholamine-induced apoptosis is mediated by activation of the beta-adrenergic signaling pathway. We tested the hypothesis that beta(1)- and beta(2)-adrenergic receptor (AR) subtypes differentially affect apoptosis in adult rat ventricular myocytes in vitro. METHODS AND RESULTS-Myocytes were first exposed to norepinephrine (NE) alone (10 mcmol/L) or NE+atenolol (AT) (10 mcmol/L) for 12 hours. AT, a beta(1)-selective AR antagonist, abolished the NE-induced increase in nick end-labeling (TUNEL)-positive cells compared with control (NE, 33+/-3% versus control, 3+/-1%, P<0.0001; NE+AT, 4+/-2% versus control, 3+/-1%, P=0. 98). Annexin V staining, DNA laddering, and caspase activity determinations corroborated these results. Subsequent experiments under prazosin treatment established the apoptosis dose-response curves for the increasingly beta(2)-selective AR agonists isoproterenol (ISO) (beta(1) approximately beta(2)) and albuterol (ALB) (beta(2)>beta(1)). ISO and ALB induced significantly less apoptosis than NE (beta(1)>beta(2)) at equimolar concentrations as assessed by TUNEL staining [1 mcmol/L: NE (8+/-2%) approximately ISO (7+/-1%)>ALB (2+/-1%); 10 mcmol/L: NE (35+/-2%)>ISO (23+/-1%)>ALB (3+/-1%); 100 mcmol/L: NE (50+/-2%)>ISO (29+/-2%)>ALB (14+/-1%), P<0.0001 except for NE versus ISO at 1 mcmol/L with P=0.62]. ALB-induced apoptosis at 100 mcmol/L was abolished by AT (10 mcmol/L), indicating a beta(1)AR-mediated effect. Importantly, ICI 118551 (0.1 mcmol/L), a highly selective beta(2)AR antagonist, did not decrease the percentage of NE-, ISO-, and ALB-induced apoptosis. Reverse transcription-polymerase chain reaction studies revealed that AT completely reversed the beta-adrenergic signaling-induced changes in the Bcl-2-to-Bax ratio. CONCLUSIONS-These observations provide evidence that beta AR-mediated apoptotic death signaling is largely dissociated from beta(2)ARs and selectively mediated by beta(1)ARs in adult rat ventricular myocytes.
背景 - 儿茶酚胺诱导的细胞凋亡是由β - 肾上腺素能信号通路的激活介导的。我们检验了这样一个假设,即β₁ - 和β₂ - 肾上腺素能受体(AR)亚型在体外对成年大鼠心室肌细胞的凋亡有不同影响。
方法与结果 - 首先将心肌细胞单独暴露于去甲肾上腺素(NE)(10 μmol/L)或NE + 阿替洛尔(AT)(10 μmol/L)中12小时。AT是一种β₁ - 选择性AR拮抗剂,与对照组相比,它消除了NE诱导的缺口末端标记(TUNEL)阳性细胞的增加(NE组为33±3%,对照组为3±1%,P < 0.0001;NE + AT组为4±2%,对照组为3±1%,P = 0.98)。膜联蛋白V染色、DNA梯状条带分析和半胱天冬酶活性测定证实了这些结果。随后在哌唑嗪处理下进行的实验建立了β₂ - 选择性逐渐增加的AR激动剂异丙肾上腺素(ISO)(β₁≈β₂)和沙丁胺醇(ALB)(β₂>β₁)的凋亡剂量反应曲线。通过TUNEL染色评估,在等摩尔浓度下,ISO和ALB诱导的细胞凋亡明显少于NE(β₁>β₂)[1 μmol/L:NE(8±2%)≈ISO(7±1%)>ALB(2±1%);10 μmol/L:NE(35±2%)>ISO(23±1%)>ALB(3±1%);100 μmol/L:NE(50±2%)>ISO(29±2%)>ALB(14±1%),除1 μmol/L时NE与ISO相比P = 0.62外,P < 0.0001]。100 μmol/L的ALB诱导的细胞凋亡被10 μmol/L的AT消除,表明这是一种β₁AR介导的效应。重要的是,高选择性β₂AR拮抗剂ICI 118551(0.1 μmol/L)并没有降低NE、ISO和ALB诱导的细胞凋亡百分比。逆转录 - 聚合酶链反应研究表明,AT完全逆转了β - 肾上腺素能信号诱导的Bcl - 2与Bax比值的变化。
结论 - 这些观察结果提供了证据,表明在成年大鼠心室肌细胞中,βAR介导的凋亡死亡信号在很大程度上与β₂ARs无关,而是由β₁ARs选择性介导的。
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