Iaccarino Guido, Izzo Raffaele, Trimarco Valentina, Cipolletta Ersilia, Lanni Francesca, Sorriento Daniela, Iovino Gianni Luigi, Rozza Francesco, De Luca Nicola, Priante Ornella, Di Renzo Gianfranco, Trimarco Bruno
Dipartimento di Medicina Clinica, Scienze Cardiovascolari ed Immunologiche, Università Federico II di Napoli, Italy.
Clin Pharmacol Ther. 2006 Dec;80(6):633-45. doi: 10.1016/j.clpt.2006.09.006.
Although blood pressure is considered the major determinant of left ventricular hypertrophy in hypertension, genetic variability is increasingly being considered among the factors influencing this complication. beta(2)-Adrenergic receptors (beta(2)ARs) are up-regulated in hypertension and largely polymorphic within the human population. Recently, we have shown that the Glu27 beta(2)AR variant is strongly associated with cardiac hypertrophy in hypertension. The objective of this study is to verify whether this polymorphism also affects hypertrophy regression in response to antihypertensive therapy.
In a prospective follow-up study we screened 970 hypertensive patients of Caucasian descent for the Gly16Arg, Gln27Glu, and Thr164Ile beta(2)AR polymorphisms and left ventricular echocardiographic hypertrophy and assigned selected patients to enalapril or atenolol to assess left ventricular hypertrophy regression after 2-year follow-up. Results were stratified according to treatment and the Glu27Gln polymorphism of the beta(2)AR. In cells with stable overexpression of the Glu27 or Gln27 variant of beta(2)AR, we also explored the implications of this polymorphism on hypertrophy-related intracellular signal transduction.
Among hypertensive patients, the Gly16 allele was found in 63% of patients and the Glu27 allele was found in 40.6%. Both polymorphisms were in linkage disequilibrium, as expected. Four hundred forty-one hypertrophic hypertensive patients completed the 2-year follow-up. At baseline, patients carrying at least 1 allele of the Glu27 variant presented with a larger cardiac size despite similar blood pressure levels (142.9 +/- 22.5 g/m(2) in Glu27 carriers versus 138.2 +/- 18.4 g/m(2) in Gln27 carriers, P < .02). Blood pressure normalization was achieved by both drugs. At follow-up, compared with the Gln27 patients, the Glu27 patients showed a larger reduction in hypertrophy when treated with enalapril (percent change in left ventricular mass, -6.3% +/- 7.7% in Glu27 carriers versus -2.18% +/- 7.9% in Gln27 carriers; P < .05) but not with atenolol therapy (-2.8% +/- 8.9% in Glu27 carriers versus -2.4% +/- 8.8% in Gln27 carriers, P = not significant). In in vitro studies the activation of p38 and extracellular signal-regulated kinase (ERK-) 1/2 (data not shown) and the activity of the atrial natriuretic factor (ANF) promoter after isoproterenol (INN, isoprenaline) stimulation were larger in Glu27 beta(2)AR overexpressing cells than in Gln27 beta(2)AR overexpressing cells (fold difference compared with unstimulated cells, 9.7 +/- 2.9 for Glu27 beta(2)AR versus 4.2 +/- 0.3 for Gln27 beta(2)AR; P < .05).
The Glu27 variant of beta(2)AR enhances hypertension-induced left ventricular hypertrophy. In these patients angiotensin-converting enzyme inhibitors are more efficient than beta-blockers in reducing cardiac size.
尽管血压被认为是高血压患者左心室肥厚的主要决定因素,但在影响这一并发症的因素中,基因变异性越来越受到关注。β₂肾上腺素能受体(β₂ARs)在高血压患者中上调,且在人群中具有高度多态性。最近,我们发现β₂AR的Glu27变体与高血压患者的心脏肥厚密切相关。本研究的目的是验证这种多态性是否也会影响抗高血压治疗后肥厚的消退。
在一项前瞻性随访研究中,我们对970名白种人高血压患者进行了Gly16Arg、Gln27Glu和Thr164Ileβ₂AR多态性及左心室超声心动图肥厚的筛查,并将部分患者分配接受依那普利或阿替洛尔治疗,以评估2年随访后的左心室肥厚消退情况。结果根据治疗方法和β₂AR的Glu27Gln多态性进行分层。在稳定过表达β₂AR的Glu27或Gln27变体的细胞中,我们还探讨了这种多态性对肥厚相关细胞内信号转导的影响。
在高血压患者中,63%的患者存在Gly16等位基因,40.6%的患者存在Glu27等位基因。正如预期的那样,这两种多态性处于连锁不平衡状态。441名肥厚性高血压患者完成了2年的随访。在基线时,携带至少1个Glu27变体等位基因的患者尽管血压水平相似,但心脏大小更大(Glu27携带者为142.9±22.5 g/m²,Gln27携带者为138.2±18.4 g/m²,P<.02)。两种药物均使血压恢复正常。在随访时,与Gln27患者相比,接受依那普利治疗的Glu27患者肥厚减轻更明显(左心室质量变化百分比,Glu27携带者为-6.3%±7.7%,Gln27携带者为-2.18%±7.9%;P<.05),但接受阿替洛尔治疗时并非如此(Glu27携带者为-2.8%±8.9%,Gln27携带者为-2.4%±8.8%,P无统计学意义)。在体外研究中,异丙肾上腺素刺激后,Glu27β₂AR过表达细胞中p38和细胞外信号调节激酶(ERK-)1/2的激活(数据未显示)以及心房利钠因子(ANF)启动子的活性均高于Gln27β₂AR过表达细胞(与未刺激细胞相比的倍数差异,Glu27β₂AR为9.7±2.9,Gln27β₂AR为4.2±0.3;P<.05)。
β₂AR的Glu27变体增强了高血压诱导的左心室肥厚。在这些患者中,血管紧张素转换酶抑制剂在减小心脏大小方面比β受体阻滞剂更有效。
