Cinaciguat, a soluble guanylate cyclase activator for the potential treatment of acute heart failure.

Juan Tamargo, Juan Duarte, Ricardo Caballero, Eva Delpón
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Abstract

The nitric oxide (NO)/soluble guanylate cyclase (sGC)/cyclic guanosine-3',5'-monophosphate (cGMP) pathway plays an important role in cardiovascular regulation by producing vasodilation and inhibiting platelet aggregation and vascular smooth muscle proliferation. The NO/SGC/cGMP pathway is disrupted in patients with heart failure as a result of a decrease in NO bioavailability and an increase in NO-insensitive forms of sGC, resulting in insufficient vasodilation. Drugs that activate sGC in a NO-independent manner may provide considerable therapeutic advantages in treating these patients. Cinaciguat (BAY-58-2667), currently in development by Bayer AG, preferentially activates sGC in its oxidized or heme-free state, when the enzyme is insensitive to both NO and nitrovasodilators. Cinaciguat exhibits potent vasodilator and antiplatelet activity, a long-lasting antihypertensive effect and a hemodynamic profile similar to that of nitrates. In clinical trials in patients with acute decompensated heart failure, cinaciguat potently unloaded the heart, increased cardiac output and renal blood flow, and preserved renal function and sodium and water excretion without further neurohumoral activation. The pharmacokinetics of cinaciguat demonstrated dose-proportionality with low individual variability and a low incidence of adverse events. The phase I and II clinical trials performed with cinaciguat so far, however, are insufficient to provide convincing evidence on the efficacy and safety of the drug. Thus, caution should be exerted before extrapolating the present preliminary data to the clinical practice.

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Cinaciguat,一种可溶鸟苷酸环化酶激活剂,用于治疗急性心力衰竭。
一氧化氮(NO)/可溶性鸟苷环化酶(sGC)/环鸟苷-3′,5′-单磷酸(cGMP)通路通过血管舒张、抑制血小板聚集和血管平滑肌增殖,在心血管调节中发挥重要作用。在心力衰竭患者中,NO/SGC/cGMP通路因NO生物利用度降低和NO不敏感SGC形式的增加而中断,导致血管舒张不足。以no独立方式激活sGC的药物可能在治疗这些患者时提供相当大的治疗优势。拜耳公司目前正在开发的Cinaciguat (BAY-58-2667)可优先激活氧化或无血红素状态的sGC,此时sGC对NO和硝基血管扩张剂都不敏感。Cinaciguat表现出有效的血管扩张和抗血小板活性,持久的降压作用和与硝酸盐相似的血流动力学特征。在急性失代偿性心力衰竭患者的临床试验中,cinaciguat有效地减轻了心脏负荷,增加了心输出量和肾血流量,并在没有进一步神经体液激活的情况下保留了肾功能和钠和水的排泄。cinaciguat的药代动力学表现出剂量正比性,个体变异性低,不良事件发生率低。然而,到目前为止,cinaciguat进行的I期和II期临床试验不足以提供令人信服的证据来证明该药物的有效性和安全性。因此,在将目前的初步数据外推到临床实践之前,应谨慎行事。
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