Exploring new treatment strategies in heart failure.

Blood pressure. Supplement Pub Date : 2000-01-01
K Swedberg
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Abstract

Heart failure remains a major and increasing cause of mortality and morbidity, even when the best available treatments are used. One of its key causes is neuroendocrine activation via the sympathetic nervous system and the renin-angiotensin system (RAS). Neuroendocrine blockers of the sympathetic nervous system (beta-blockers) and of the RAS (angiotensin-converting enzyme [ACE] inhibitors and angiotensin II type 1 [AT1] receptor blockers) therefore have an important potential therapeutic role in heart failure. The promising results from clinical trials with beta-blockers suggest that these drugs will become an established part of the future management of patients with mild to moderate symptomatic heart failure. Blockade of the RAS with ACE inhibitors has also been shown to be effective in reducing the risk of morbidity and mortality in patients with heart failure. Blockade of the AT1-receptor, with agents such as candesartan, produces more specific and, theoretically, more complete blockade of the major negative cardiovascular effects of angiotensin II than is possible using ACE inhibitors, whilst maintaining placebo-like tolerability. Furthermore, AT1-receptor blockade leads to increased stimulation of the angiotensin II type 2 (AT2) receptor, which, according to experimental data, may have favourable cardiovascular effects. Following encouraging results from two pilot studies, a major new international study programme - CHARM (Candesartan in Heart failure - Assessment of Reduction in Mortality and morbidity) - has been initiated to define the clinical benefits of candesartan cilexetil in a wide variety of patients with symptomatic heart failure. CHARM is the first study to accept all relevant heart failure patients who may benefit from RAS blockade, irrespective of their left ventricular function or tolerance of ACE inhibitors. The 6500 patients to be recruited will be divided among three integrated outcome studies. Two of these studies will examine the effect of candesartan cilexetil versus placebo in patients with an ejection fraction of 40% or less who are tolerant or intolerant of ACE inhibitors. The third study arm will examine the benefits of candesartan cilexetil in a previously seldom studied group: those with symptomatic heart failure, but with preserved left-ventricular systolic function. Recruitment of patients into the study has started.

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探索心力衰竭的新治疗策略。
即使采用了现有的最佳治疗方法,心力衰竭仍然是死亡率和发病率的一个主要和日益增加的原因。其主要原因之一是通过交感神经系统和肾素血管紧张素系统(RAS)激活神经内分泌。因此,交感神经系统的神经内分泌阻滞剂(β -阻滞剂)和RAS(血管紧张素转换酶[ACE]抑制剂和血管紧张素II型1 [AT1]受体阻滞剂)在心力衰竭中具有重要的潜在治疗作用。β受体阻滞剂临床试验的令人鼓舞的结果表明,这些药物将成为未来轻度至中度症状性心力衰竭患者治疗的既定部分。用ACE抑制剂阻断RAS也被证明可以有效降低心力衰竭患者的发病率和死亡率。与使用ACE抑制剂相比,坎地沙坦等药物阻断at1受体,在保持安慰剂样耐受性的同时,对血管紧张素II的主要负面心血管效应产生更特异性和理论上更完全的阻断。此外,at1受体阻断导致血管紧张素II 2型(AT2)受体的刺激增加,根据实验数据,这可能对心血管有有利的影响。在两项试点研究取得令人鼓舞的结果之后,一项新的重大国际研究项目——坎地沙坦在心力衰竭中的应用——死亡率和发病率降低评估——已经启动,以确定坎地沙坦西列地酯在各种症状性心力衰竭患者中的临床益处。CHARM是首个接受所有可能受益于RAS阻断的相关心力衰竭患者的研究,无论其左心室功能或对ACE抑制剂的耐受性如何。将招募的6500名患者将分为三个综合结果研究。其中两项研究将检查坎地沙坦西列地酯与安慰剂在射血分数为40%或更低、ACE抑制剂耐受或不耐受的患者中的效果。第三组研究将检查坎地沙坦西列地酯在以前很少研究的人群中的益处:有症状性心力衰竭但左心室收缩功能保留的人群。该研究的患者招募工作已经开始。
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