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Impact of increased heart rate on clinical outcomes in hypertension: implications for antihypertensive drug therapy.

机译:心率增加对高血压临床预后的影响:对降压药物治疗的影响。

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Thirty-eight studies have been published to date on the association between elevated heart rate and mortality. After adjustment for other risk factors, only two studies for all-cause mortality and four studies for cardiovascular mortality reported an absence of association between heart rate and mortality in male populations. This relationship has been found to be generally weaker among females. Most of these studies investigated samples of general populations. The four studies performed in hypertensive men found a positive association between heart rate and all-cause mortality (hazard ratios ranging from 1.9 to 2.0) or cardiovascular mortality (hazard ratios ranging from 1.3 to 1.7). In spite of this evidence, elevated heart rate remains a neglected cardiovascular risk factor in both genders. The pathogenetic mechanisms connecting high heart rate, hypertension, atherosclerosis and cardiovascular events have also been explicated in many studies. Elevated heart rate is due to an increased sympathetic and decreased parasympathetic tone. This altered balance of the autonomic nervous system tone could explain the increase in events with the increased heart rate. However, it has also been proved that blood flow changes associated with high heart rate favour both the formation of the atherosclerotic lesion and the occurrence of the cardiovascular event. Reduction of heart rate in hypertensive patients with increased heart rate could be an additional goal of antihypertensive therapy. Several trials retrospectively showed the beneficial effect of cardiac-slowing drugs, such as beta-adrenoceptor antagonists (beta-blockers) and non-dihydropyridine calcium channel antagonists, on mortality, notably in patients with coronary heart disease, but no published data are available in patients with hypertension free of coronary heart disease. Other antihypertensive drugs that have been shown to reduce the heart rate are centrally acting drugs and angiotensin II receptor antagonists, but their bradycardic effect is rather weak. The f-channel antagonist ivabradine is a selective heart rate-lowering agent with no effect on blood pressure. Although it has not been proven in existing trials, it would seem reasonable to recommend antihypertensive agents that decrease the heart rate in hypertensive patients with a heart rate higher than 80-85 beats per minute. Since the fast heart rate per se causes cardiovascular damage, all drugs that lower the heart rate have the potential of further reducing cardiovascular events in patients with elevated heart rate. Unfortunately, lowering of the heart rate is not a clinically recognised goal. Prospective trials investigating whether treatment of high heart rate can prevent cardiovascular events, notably in hypertensive patients, are warranted.
机译:迄今为止,已发表了38篇关于心率升高与死亡率之间关系的研究。在调整了其他风险因素后,只有两项针对全因死亡率的研究和针对心血管疾病死亡率的四项研究报告说,男性人群中心率与死亡率之间没有关联。已经发现这种关系在女性中通常较弱。这些研究大多数调查了普通人群的样本。在高血压男性中进行的四项研究发现,心率与全因死亡率(危险比在1.9至2.0之间)或心血管疾病死亡率(危险比在1.3至1.7之间)之间呈正相关。尽管有这些证据,但心率升高仍然是男女双方被忽略的心血管危险因素。许多研究还阐明了与高心率,高血压,动脉粥样硬化和心血管事件有关的致病机制。心律升高是由于交感神经增加和副交感神经减少。自主神经系统音调的这种平衡改变可能解释了随着心率增加事件的增加。然而,也已经证明与高心率相关的血流变化有利于动脉粥样硬化病变的形成和心血管事件的发生。降低心率升高的高血压患者的心率可能是降压治疗的另一个目标。数项试验回顾性地显示了诸如β-肾上腺素能受体拮抗剂(β-受体阻滞剂)和非二氢吡啶类钙离子通道拮抗剂之类的减慢心律药物对死亡率的有益作用,特别是在冠心病患者中,但尚无相关数据发表。高血压患者无冠心病。已显示可降低心律的其他降压药是中枢性药物和血管紧张素II受体拮抗剂,但它们的心动过缓作用较弱。 F通道拮抗剂伊伐布雷定是一种选择性的降低心率的药物,对血压没有影响。尽管尚未在现有试验中得到证实,但建议使用降压药降低心率高于每分钟80-85次搏动的高血压患者的心率,这似乎是合理的。由于心率过快本身会导致心血管损害,因此所有降低心率的药物都有可能进一步减少心率升高患者的心血管事件。不幸的是,降低心率并不是临床上公认的目标。有必要进行前瞻性研究,以调查高心率治疗是否可以预防心血管事件,特别是在高血压患者中。

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