如果伊伐布雷定抑制通道不能改善实验性脓毒症休克中的心脏和血管功能。

If Channel Inhibition With Ivabradine Does Not Improve Cardiac and Vascular Function in Experimental Septic Shock.

作者信息

Wei Chaojie, Al Kattani Narimane, Louis Huguette, Albuisson Eliane, Levy Bruno, Kimmoun Antoine

机构信息

*INSERM U 1116, Groupe Choc, Equipe 2, Faculté de Médecine, Vandoeuvre les Nancy, France †Université de Lorraine, Nancy, France ‡INSERM U 1116, Equipe 1, Faculté de Médecine, Vandoeuvre les Nancy, France §Unité ESPRI-BioBase, CHRU Nancy, Vandoeuvre les Nancy, France ¶CHU Nancy, Service de Réanimation Médicale Brabois, Pole Cardiovasculaire et Réanimation Médicale, Hôpital Brabois, Vandoeuvre les Nancy, France.

出版信息

Shock. 2016 Sep;46(3):297-303. doi: 10.1097/SHK.0000000000000593.

DOI:10.1097/SHK.0000000000000593

PMID:26909707

Abstract

OBJECTIVE

Previous studies have suggested that lowering heart rate (HR) by selective β1-blockers improves sepsis-induced cardiac and vascular dysfunction primarily by decreasing proinflammatory pathways. However, the impact of isolated heart rate reduction (HRR) on hemodynamics and inflammatory pathways remains unknown. The present study was designed to assess the effects of HRR by ivabradine, an If channel inhibitor, on cardiovascular function and inflammatory pathways in peritonitis-induced septic shock in rats.

DESIGN

Randomized animal study.

SETTING

University research laboratory.

INTERVENTIONS

Four hours after cecal ligation and puncture (CLP), Wistar rats were randomly allocated to the following groups: CLP (n = 8) and CLP + ivabradine (n = 8, administered per os 4 h after the surgery). Another eight Wistar male rats underwent sham operation. All rats received a continuous infusion of saline (10 mL kg h), analgesic (nalbuphine: 0.2 mg kg h), and antibiotics (imipenem and cilastatin sodium: 10 mg kg) 4 h after the surgery. Assessment at 18 h included hemodynamics, in vivo cardiac function by echocardiography, and ex vivo vasoreactivity by myography. Circulating cytokine levels (TNF-α, IL-6, and IL-10) were measured by ELISA, whereas cardiac and vascular protein expressions of NF-κB/IκBα/iNOS and Akt/eNOS were assessed by Western blotting.

RESULTS

Compared with sham animals, CLP induced tachycardia, hypotension, decreased cardiac output, hyperlactatemia, and vascular hyporesponsiveness to vasopressors. Compared with the CLP group, adjunction of ivabradine decreased the HR without any impact on blood pressure, lactatemia, or vascular responsiveness to vasopressors. Adjunction of ivabradine to CLP rats had no impact on TNF-α, IL-6, and IL-10 cytokines, or on the protein expression levels of phosphorylated forms of NF-κB, Akt, eNOS, and degradation of IκBα in cardiac and vascular tissues.

CONCLUSION

Isolated HRR by ivabradine in an experimental model of septic shock does not appear to be associated with any effect on the tested parameters of cardiac function or on vascular responsiveness to vasopressors. Moreover, in this setting, ivabradine does not alter the circulating levels of selected pro/anti-inflammatory cytokines or cardiac and vascular NF-κB/IκBα protein expression levels.

摘要

目的

以往研究表明，选择性β1受体阻滞剂降低心率（HR）主要通过减少促炎途径来改善脓毒症诱导的心脏和血管功能障碍。然而，单纯降低心率（HRR）对血流动力学和炎症途径的影响尚不清楚。本研究旨在评估If通道抑制剂伊伐布雷定降低心率（HRR）对大鼠腹膜炎诱导的感染性休克心血管功能和炎症途径的影响。

设计

随机动物研究。

地点

大学研究实验室。

干预措施

在盲肠结扎和穿刺（CLP）4小时后，将Wistar大鼠随机分为以下几组：CLP组（n = 8）和CLP +伊伐布雷定组（n = 8，术后4小时口服给药）。另外8只Wistar雄性大鼠接受假手术。所有大鼠在术后4小时接受生理盐水（10 mL·kg-1·h-1）、镇痛药（纳布啡：0.2 mg·kg-1·h-1）和抗生素（亚胺培南和西司他丁钠：10 mg·kg-1）的持续输注。18小时时的评估包括血流动力学、超声心动图评估体内心脏功能以及肌张力测定评估离体血管反应性。通过酶联免疫吸附测定法（ELISA）测量循环细胞因子水平（TNF-α、IL-6和IL-10），而通过蛋白质免疫印迹法评估心脏和血管中NF-κB/IκBα/iNOS以及Akt/eNOS的蛋白质表达。

结果

与假手术动物相比，CLP诱导心动过速、低血压、心输出量降低、高乳酸血症以及血管对血管升压药反应性降低。与CLP组相比，伊伐布雷定的加入降低了心率，而对血压、乳酸血症或血管对血管升压药的反应性没有影响。在CLP大鼠中加入伊伐布雷定对TNF-α、IL-6和IL-10细胞因子，或对心脏和血管组织中NF-κB、Akt、eNOS磷酸化形式的蛋白质表达水平以及IκBα的降解没有影响。