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在临床前心力衰竭模型中,通过选择性 V2 受体拮抗与双重 V2/V1a 受体拮抗来区分精氨酸加压素的拮抗作用。

Differentiation of arginine vasopressin antagonistic effects by selective V2 versus dual V2/V1a receptor blockade in a preclinical heart failure model.

机构信息

Bayer Health Care, Cardiovascular Research Institute, Wuppertal, Germany.

出版信息

Am J Ther. 2011 Jan;18(1):31-7. doi: 10.1097/MJT.0b013e3181f890ad.

Abstract

Arginine vasopressin (AVP) is increased in patients with heart failure (HF). Its actions are linked to free water reabsorption (V2-) and arteriolar vasoconstriction (V1a receptor). AVP can exacerbate the cardiorenal syndrome with excess fluid retention and afterload increase. Tolvaptan (TOL; selective V2 antagonist) and Conivaptan (CON; dual V1a/V2 antagonist) are two AVP antagonists that counteract the action of AVP with distinct profiles. We investigated the therapeutic effects of CON and TOL in an acute HF model. Mongrel dogs were paced continuously at 220 beats/min. After 14 days, the animals underwent acute testing. Dogs were instrumented to measure cardiac output, blood pressure, pulmonary artery pressure, and left ventricular dP/dtmax. Additionally, during the acute experiments, vasopressin was infused intravenously (4 mU/kg/min) to achieve constant and controlled pathophysiological levels of AVP. Subsequently, animals received either CON or TOL (n = 6; 0.1-mg/kg bolus). There were no significant differences in effect on mean arterial pressure, dP/dtmax, central venous pressure, and urine output between CON and TOL. In contrast, cardiac output increased by 0.15 l/min after CON and decreased by 0.6 l/min after TOL (P < 0.01). Accordingly, the total peripheral resistance increased after TOL by 250 dyns/cm and decreased after CON by 125 dyns/cm (P < 0.01). In conclusion, it was demonstrated that in an acute HF model, CON lowered, whereas TOL increased afterload. The results suggest that dual V1a/V2 blockade in the acute HF setting could be beneficial compared with selective V2 blockade. Chronic experiments are needed to determine whether this finding can translate into a sustained clinical advantage.

摘要

精氨酸加压素(AVP)在心力衰竭(HF)患者中增加。它的作用与游离水重吸收(V2-)和小动脉血管收缩(V1a 受体)有关。AVP 可通过过多的液体潴留和后负荷增加加重心肾综合征。托伐普坦(TOL;选择性 V2 拮抗剂)和康维普坦(CON;双重 V1a/V2 拮抗剂)是两种 AVP 拮抗剂,它们通过不同的特性来对抗 AVP 的作用。我们研究了 CON 和 TOL 在急性 HF 模型中的治疗效果。杂种狗以 220 次/分的速度持续起搏。14 天后,动物进行急性测试。对狗进行仪器操作以测量心输出量、血压、肺动脉压和左心室 dp/dtmax。此外,在急性实验中,静脉内输注加压素(4mU/kg/min)以达到恒定和受控的生理 AVP 水平。随后,动物接受 CON 或 TOL(n=6;0.1mg/kg 推注)。CON 和 TOL 对平均动脉压、dp/dtmax、中心静脉压和尿量的影响没有显著差异。相反,CON 后心输出量增加 0.15l/min,TOL 后减少 0.6l/min(P<0.01)。相应地,TOL 后总外周阻力增加 250dyns/cm,CON 后减少 125dyns/cm(P<0.01)。总之,在急性 HF 模型中,CON 降低而 TOL 增加后负荷。结果表明,在急性 HF 环境中,双重 V1a/V2 阻断可能比选择性 V2 阻断更有益。需要进行慢性实验以确定这一发现是否能转化为持续的临床优势。

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