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Vasopressin in vasodilatory shock: hemodynamic stabilization at the cost of the liver and the kidney?

机译:血管舒张性休克中的加压素:以血流动力学稳定为代价以肝肾为代价吗?

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摘要

Infusing arginine vasopressin (AVP) in advanced vasodilatory shock is usually accompanied by a decrease in cardiac index and systemic oxygen transport. Whether or not such a vasoconstriction impedes regional blood flow and thus visceral organ function, even when low AVP is used, is still a matter of debate. Krejci and colleagues now report, in this issue of Critical Care, that infusing 'low-dose' AVP during early, short-term, normotensive and normodynamic fecal peritonitis-induced porcine septicemia markedly reduced both renal and portal blood flow, and consequently total hepatic blood flow, whereas hepatic arterial flow was not affected. This macrocirculatory response was concomitant with reduced kidney microcirculatory perfusion, whereas liver micro-circulation remained unchanged. From these findings the authors conclude that the use of AVP to treat hypotension should be cautioned against in patients with septic shock. Undoubtedly, given its powerful vasoconstrictor properties, which are not accompanied by positive inotropic qualities (in contrast with most of the equally potent standard care 'competitors', namely catecholamines), the safety of AVP is still a matter of concern. Nevertheless, the findings reported by Krejci and colleagues need to be discussed in the context of the model design, the timing and dosing of AVP as well as the complex interaction between visceral organ perfusion and function.
机译:在晚期血管舒张性休克中注入精氨酸加压素(AVP)通常伴有心脏指数降低和全身氧转运减少。即使使用低AVP,这种血管收缩是否会阻碍局部血流,从而阻碍内脏器官功能,仍是一个有争议的问题。 Krejci及其同事现在在本期《重症监护》中报告说,在早期,短期,血压正常和正常血流性大便性腹膜炎引起的猪败血症中注入“低剂量” AVP显着降低了肾脏和门脉血流量,因此全肝血流,而肝动脉血流不受影响。这种大循环反应伴随着肾脏微循环灌注的减少,而肝脏微循环保持不变。从这些发现中,作者得出结论,败血性休克患者应警惕使用AVP治疗低血压。毫无疑问,鉴于其强大的血管收缩特性,并没有积极的正性肌力特性(与大多数同等效力的标准护理“竞争者”,即儿茶酚胺相比),AVP的安全性仍然值得关注。尽管如此,仍需要在模型设计,AVP的时机和剂量以及内脏器官灌注与功能之间复杂的相互作用的背景下讨论Krejci及其同事报告的发现。

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