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心钠肽和脑钠肽在心力衰竭患者中的病理生理意义及临床应用

Pathophysiological significance and clinical application of ANP and BNP in patients with heart failure.

作者信息

Yoshimura M, Yasue H, Ogawa H

机构信息

Department of Cardiovascular Medicine, Kumamoto University School of Medicine, Japan.

出版信息

Can J Physiol Pharmacol. 2001 Aug;79(8):730-5.

Abstract

Plasma levels of ANP and BNP increase in accordance with the severity of the heart failure. In severe cases, the amount of BNP secreted surpasses that of ANP. The main secretion site of BNP is the ventricles, and that of ANP is the atria. However, ANP is also secreted from the ventricles as heart failure advances, and thus the ventricles are important sites for both BNP and ANP. It is well known that myocardial stretch is a key factor in the stimulation of the secretion of ANP and BNP, although neurohumoral factors also play a role in the secretion mechanism. The major physiological effects of ANP and BNP are vasodilation, natriuresis, and inhibition of the renin-angiotensin-aldosterone (RAA) and the sympathetic nervous systems; all of which are supposed to suppress the progression of heart failure. The inhibitory action of ANP and BNP on the RAA system has been considered to be an extra-cardiac effect. We recently reported the activation of an angiotensin-converting enzyme and aldosterone production in failing human hearts. ANP and BNP, however, would inhibit aldosterone production, not only in the adrenal cortex but also in cardiac tissue. ANP, and especially BNP, are useful markers of the heart's status during treatment for heart failure. The infusion of synthetic ANP (hANP) or BNP (Nesiritide) is effective in the treatment of acute heart failure. In Japan, BNP occupies an important position in the diagnosis of chronic heart failure, as ANP does in the treatment of acute heart failure.

摘要

心房钠尿肽(ANP)和脑钠肽(BNP)的血浆水平会随着心力衰竭的严重程度而升高。在严重病例中,BNP的分泌量超过ANP。BNP的主要分泌部位是心室,而ANP的主要分泌部位是心房。然而,随着心力衰竭的进展,心室也会分泌ANP,因此心室是BNP和ANP的重要分泌部位。众所周知,心肌牵张是刺激ANP和BNP分泌的关键因素,尽管神经体液因素在分泌机制中也起作用。ANP和BNP的主要生理作用是血管舒张、利钠以及抑制肾素-血管紧张素-醛固酮(RAA)系统和交感神经系统;所有这些都被认为可以抑制心力衰竭的进展。ANP和BNP对RAA系统的抑制作用被认为是一种心脏外效应。我们最近报道了在衰竭的人类心脏中血管紧张素转换酶的激活和醛固酮的产生。然而,ANP和BNP不仅会抑制肾上腺皮质中的醛固酮产生,也会抑制心脏组织中的醛固酮产生。ANP,尤其是BNP,是心力衰竭治疗期间心脏状态的有用标志物。输注合成的ANP(hANP)或BNP(奈西立肽)对急性心力衰竭的治疗有效。在日本,BNP在慢性心力衰竭的诊断中占据重要地位,就如同ANP在急性心力衰竭的治疗中一样。

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