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早期吸入依前列醇治疗对左心室辅助装置植入期间肺动脉压力和失血的影响。

Effects of early inhaled epoprostenol therapy on pulmonary artery pressure and blood loss during LVAD placement.

作者信息

Groves Danja S, Blum Franziska E, Huffmyer Julie L, Kennedy Jamie L W, Ahmad Hasan B, Durieux Marcel E, Kern John A

机构信息

Department of Anesthesiology, Division of Cardiac, Thoracic and Vascular Surgery, University of Virginia Health Systems, Charlottesville, VA.

Department of Anesthesiology, Division of Cardiac, Thoracic and Vascular Surgery, University of Virginia Health Systems, Charlottesville, VA.

出版信息

J Cardiothorac Vasc Anesth. 2014 Jun;28(3):652-60. doi: 10.1053/j.jvca.2013.05.028. Epub 2013 Oct 5.

Abstract

OBJECTIVE

Several strategies have been used to reduce the incidence of right ventricular failure after left ventricular assist device (LVAD) placement, including pulmonary vasodilation. The inhaled prostacyclin, epoprostenol, selectively dilates the pulmonary vasculature of ventilated areas of the lung, but also has been shown to inhibit platelet aggregation.(1) The authors evaluated the impact of early initiation of epoprostenol administration during LVAD placement on pulmonary artery pressures, use of vasoactive drugs, and blood loss.

DESIGN

Retrospective data review.

SETTING

Single center, university hospital.

PARTICIPANTS

A total of 37 consecutive patients undergoing LVAD (HeartMate II) placement were included.

INTERVENTIONS

In the first group of 23 patients (group 1), inhaled epoprostenol was not initiated until weaning from cardiopulmonary bypass (CPB). In a subsequent group of 14 patients (group 2), inhaled epoprostenol was started shortly after induction of anesthesia and continued throughout and post-CPB.

MEASUREMENTS

Mean and systolic pulmonary artery pressures (mPAP, sPAP), vasoactive drugs, as well as hemodynamic parameters, blood loss, and use of blood products were recorded at the following time points: Baseline (BL), pre-CPB, post-CPB, and during postoperative days (POD) 0, 1, and 2. Data are presented as mean±SD or median [25%, 75%].

RESULTS

Groups did not differ in demographic characteristics and comorbidities. BL sPAP (41±13 v 46±15 mmHg; p = 0.051) and mPAP (32±8 v 34±8 mmHg; p = 0.483) values were not different between the groups. Systolic and mPAP in group 1 were significantly lower in the postoperative period compared with BL (sPAP on POD 0: 34±6 mmHg; p<0.001; mPAP on POD 0, 1, and 2: 24±4 mmHg, 25±4 mmHg, 27±6 mmHg; p<0.001-0.003)). In contrast, in group 2, sPAP as well as mPAP were significantly lower during weaning from CPB (sPAP: 37±8; p = 0.002; mPAP: 28±5 mmHg; p = 0.016) as well as in the postoperative period (sPAP on POD 0, 1 and 2: 34±7, 35±7, and 37±10 mmHg; p<0.001-0.004; mPAP on POD 0, 1, and 2: 24±4 mmHg, 25±5 mmHg, 27±6 mmHg; p<0.001-0.006). Blood loss on postoperative day 0 was significantly lower in group 1 (1646 mL [1137, 2300] v 2915 mL [2335, 6155]; p = 0.006). Epoprostenol was a significant predictor of blood loss in the regression model (p<0.001) but did not predict a change in sPAP.

CONCLUSIONS

Inhaled prostacyclin reduces sPAP and mPAP in the postoperative period after LVAD placement regardless of the timing of initiation. Early initiation seems to reduce sPAP as well as mPAP more effectively during the weaning process from CPB. However, early initiation is associated with an increased blood loss in the immediate postoperative period. The concept of preventively "bathing" the lung in prostacyclin should be evaluated critically in a prospective fashion to adequately examine this question.

摘要

目的

已采用多种策略来降低左心室辅助装置(LVAD)植入后右心室衰竭的发生率,包括肺血管扩张。吸入性前列环素依前列醇可选择性扩张肺通气区域的肺血管,但其也已被证明可抑制血小板聚集。(1)作者评估了在LVAD植入期间早期开始使用依前列醇对肺动脉压力、血管活性药物使用及失血的影响。

设计

回顾性数据审查。

设置

单中心大学医院。

参与者

共纳入37例连续接受LVAD(HeartMate II)植入的患者。

干预措施

在第一组23例患者(第1组)中,直到脱离体外循环(CPB)才开始吸入依前列醇。在随后的14例患者组(第2组)中,麻醉诱导后不久即开始吸入依前列醇,并在CPB期间及CPB后持续使用。

测量

在以下时间点记录平均和收缩期肺动脉压力(mPAP、sPAP)、血管活性药物以及血流动力学参数、失血量和血液制品的使用情况:基线(BL)、CPB前、CPB后以及术后第0、1和2天。数据以平均值±标准差或中位数[25%,75%]表示。

结果

两组在人口统计学特征和合并症方面无差异。两组间的基线sPAP(41±13对46±15 mmHg;p = 0.051)和mPAP(32±8对34±8 mmHg;p = 0.483)值无差异。与基线相比,第1组术后收缩期和mPAP显著降低(术后第0天sPAP:34±6 mmHg;p<0.001;术后第0、1和2天mPAP:24±4 mmHg、25±4 mmHg、27±6 mmHg;p<0.001 - 0.003)。相比之下,在第2组中,CPB脱机期间sPAP和mPAP均显著降低(sPAP:37±8;p = 0.002;mPAP:28±5 mmHg;p = 0.016),术后期间也显著降低(术后第0、1和2天sPAP:34±7、35±7和37±10 mmHg;p<0.001 - 0.004;术后第0、1和2天mPAP:24±4 mmHg、25±5 mmHg、27±6 mmHg;p<0.001 - 0.006)。第1组术后第0天的失血量显著低于第2组(1646 mL [1137, 2300]对2915 mL [2335, 6155];p = 0.006)。在回归模型中,依前列醇是失血量的显著预测因子(p<0.001),但不能预测sPAP的变化。

结论

无论开始使用的时机如何,吸入性前列环素均可降低LVAD植入术后的sPAP和mPAP。早期开始使用似乎在CPB脱机过程中更有效地降低sPAP和mPAP。然而,早期开始使用与术后即刻失血量增加有关。应以前瞻性方式严格评估在前列环素中预防性“灌注”肺的概念,以充分研究这个问题。

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