Present and future pharmacotherapy for heart failure

Doggrell, Sheila A; Brown, Lindsay

doi:10.1517/14656566.3.7.915

Cited by 14 publications

(1 citation statement)

References 108 publications

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“…A large‐scale trial (OVERTURE) of the vasopeptidase inhibitor omapatrilat (with dual actions of inhibiting both ACE and neutral endopeptidase) showed that omapatrilat was no more effective than the conventional ACE inhibitor lisinopril for treatment of patients with moderate to severe chronic heart failure 59,60 . Similarly, a large‐scale trial testing inhibition of the inflammatory mediator tumour necrosis factor‐α (TNF‐α) with etanerccpt (a soluble TNF receptor preparation thought to inactivate TNF‐α when given intravenously) was terminated early for lack of benefits, as was also the case for infliximab, another TNF‐α antagonist 61–63 . TNF‐α inhibition no longer appears to be a viable strategy for treatment of heart failure.…”

Section: Testing New Strategiesmentioning

confidence: 99%

Levosimendan: A New Dual‐action Drug in the Treatment of Acute Heart Failure

Mebazaa

Erhardt

2003

Int J Clinical Practice

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SUMMARYLevosimendan is a new agent for the treatment of acute heart failure. Levosimendan acts via complementary mechanisms; it enhances contractility by sensitising cardiac myofilaments to calcium and dilates blood vessels by opening ATP‐dependent potassium channels. In contrast to traditional inotropes (β‐agonists or phosphodiesterase inhibitors), levosimendan does not raise myocyte calcium levels and is therefore less likely to elicit arrhythmias or to impair diastolic relaxation. The clinical efficacy of levosimendan is supported by four key clinical studies, including more than 900 patients hospitalised for cardiac decompensation due to acutely worsened chronic heart failure or to heart failure following myocardial infarction. When given as short‐term therapy, levosimendan enhances cardiac output, reduces systemic vascular resistance and lowers pulmonary capillary wedge pressure. At 31 days post‐treatment, mortality rates were halved in decompensated chronic heart failure patients who received levosimendan, compared with those on dobutamine – an advantage sustained at 180 days. Similar survival gains were observed among acute failure patients treated with levosimendan following myocardial infarction. With its substantial haemodynamic and survival benefits, levosimendan is well suited to be part of routine management for patients with acutely decompensated heart failure.

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Section: Testing New Strategiesmentioning

confidence: 99%

Levosimendan: A New Dual‐action Drug in the Treatment of Acute Heart Failure

Mebazaa

Erhardt

2003

Int J Clinical Practice

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Down-regulation of sodium current in chronic heart failure: effect of long-term therapy with carvedilol

Maltsev¹,

Sabbah²,

Undrovinas³

2002

Cellular and Molecular Life Sciences (CMLS)

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Evidence has accumulated recently about the importance of alterations in Na+ channel function and slow myocardial conduction for arrhythmias in the infarcted and failing heart. The present study tested a hypothesis that Na+ current (INa/C) density decreases in chronic heart failure (HF) and that Na+ channel (NaCh) functional density can be restored by long-term therapy with carvedilol, a mixed alpha- and beta-adrenergic blocker. Studies were performed using a canine model of chronic HF produced in dogs by sequential intracoronary embolizations with microspheres. HF developed approximately 3 months after the last embolization (left ventricle, LV, ejection fraction = 28 +/- 1%). Ventricular cardiomyocytes (VCs) were isolated enzymatically from LV mid-myocardium, and INa was measured by whole-cell patch-clamp. The maximum INa/C was decreased in failing (n = 19) compared to normal (n = 12) hearts (33.1 +/- 1.6 vs 48.5 +/- 5.1 pA/pF, mean +/- SE, p < 0.001). The steady-state inactivation and activation of INa remained unchanged in failing compared to normal hearts. Long-term treatment with carvedilol (1 mg/kg, twice daily for 3 months) normalized INa/C in dogs with HF. INa/C in HF dogs (n = 6) treated with carvedilol was higher compared to that of non-treated HF dogs (n = 6) (49.4 +/- 0.9 vs 29 +/- 4.8 pA/pF, p < 0.007). In vitro culture of VCs of failing hearts for 24 h did not restore INa/C. However, INa/C was partially restored when VCs were incubated for 24 h with BAPTA-AM, an intracellular Ca2+ buffer. Thus, we conclude that experimental chronic HF in dogs results in down-regulation of the functional density of NaCh that can be restored by long-term therapy with carvedilol. The mechanism of NaCh down-regulation in HF may be linked to poor Ca2+ handling in this stage of disease.

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