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基线呼吸机参数对接受静脉-静脉体外膜肺氧合治疗的急性呼吸窘迫综合征患者住院死亡率的影响:一项回顾性队列研究。

The impacts of baseline ventilator parameters on hospital mortality in acute respiratory distress syndrome treated with venovenous extracorporeal membrane oxygenation: a retrospective cohort study.

机构信息

Department of Cardiovascular Surgery, Chang Gung Memorial Hospital and Chang Gung University, Taoyuan, Taiwan.

School of Traditional Chinese Medicine, Chang Gung University, Taoyuan, Taiwan.

出版信息

BMC Pulm Med. 2017 Dec 8;17(1):181. doi: 10.1186/s12890-017-0520-5.

Abstract

BACKGROUND

Venovenous extracorporeal membrane oxygenation (VV-ECMO) is a valuable life support in acute respiratory distress syndrome (ARDS) in adult patients. However, the success of VV-ECMO is known to be influenced by the baseline settings of mechanical ventilation (MV) before its institution. This study was aimed at identifying the baseline ventilator parameters which were independently associated with hospital mortality in non-trauma patients receiving VV-ECMO for severe ARDS.

METHODS

This retrospective study included 106 non-trauma patients (mean age: 53 years) who received VV-ECMO for ARDS in a single medical center from 2007 to 2016. The indication of VV-ECMO was severe hypoxemia (PO/ FiO ratio < 70 mmHg) under pressure-controlled MV with peak inspiratory pressure (PIP) > 35 cmHO, positive end-expiratory pressure (PEEP) > 5 cmHO, and FO > 0.8. Important demographic and clinical data before and during VV-ECMO were collected for analysis of hospital mortality.

RESULTS

The causes of ARDS were bacterial pneumonia (n = 41), viral pneumonia (n = 24), aspiration pneumonitis (n = 3), and others (n = 38). The median duration of MV before ECMO institution was 3 days and the overall hospital mortality was 53% (n = 56). The medians of PaO/ FiO ratio, PIP, PEEP, and dynamic pulmonary compliance (PC) at the beginning of MV were 84 mmHg, 32 cmHO, 10 cmHO, and 21 mL/cmHO, respectively. However, before the beginning of VV-ECMO, the medians of PaO/ FiO ratio, PIP, PEEP, and PC became 69 mmHg, 36 cmHO, 14 cmHO, and 19 mL/cmHO, respectively. The escalation of PIP and the declines in PaO/ FiO ratio and PC were significantly correlated with the duration of MV before ECMO institution. Finally, the duration of MV (OR: 1.184, 95% CI: 1.079-1.565, p < 0.001) was found to be the only baseline ventilator parameter that independently affected the hospital mortality in these ECMO-treated patients.

CONCLUSION

Since the duration of MV before ECMO institution was strongly correlated to the outcome of adult respiratory ECMO, medical centers are suggested to find a suitable prognosticating tool to determine the starting point of respiratory ECMO among their candidates with different duration of MV.

TRIAL REGISTRATION

This study reported a health care intervention on human participants and was retrospectively registered. The Chang Gung Medical Foundation Institutional Review Board approved the study (no. 201601483B0 ) on November 23, 2016. All of the data were extracted from December 1, 2016, to January 31, 2017.

摘要

背景

体外膜肺氧合(VV-ECMO)是治疗成人急性呼吸窘迫综合征(ARDS)的一种有价值的生命支持手段。然而,VV-ECMO 的成功与否已知受到其启动前机械通气(MV)的基线设置的影响。本研究旨在确定在单一医疗中心接受 VV-ECMO 治疗的非创伤性严重 ARDS 患者中,与住院死亡率独立相关的基线呼吸机参数。

方法

本回顾性研究纳入了 2007 年至 2016 年期间在单一医疗中心因 ARDS 接受 VV-ECMO 的 106 例非创伤性患者(平均年龄:53 岁)。VV-ECMO 的适应证为压力控制 MV 下严重低氧血症(PO/FiO 比值<70mmHg),同时伴有峰值吸气压力(PIP)>35cmHO、呼气末正压(PEEP)>5cmHO 和 FO>0.8。收集 VV-ECMO 前和期间的重要人口统计学和临床数据,以分析住院死亡率。

结果

ARDS 的病因分别为细菌性肺炎(n=41)、病毒性肺炎(n=24)、吸入性肺炎(n=3)和其他(n=38)。MV 前 ECMO 机构的中位持续时间为 3 天,总住院死亡率为 53%(n=56)。MV 开始时的 PaO/FiO 比值、PIP、PEEP 和动态肺顺应性(PC)中位数分别为 84mmHg、32cmHO、10cmHO 和 21mL/cmHO。然而,在开始 VV-ECMO 之前,PaO/FiO 比值、PIP、PEEP 和 PC 的中位数分别变为 69mmHg、36cmHO、14cmHO 和 19mL/cmHO。PIP 的升高和 PaO/FiO 比值和 PC 的下降与 ECMO 前 MV 的持续时间显著相关。最后,MV 持续时间(OR:1.184,95%CI:1.079-1.565,p<0.001)被发现是唯一独立影响这些 ECMO 治疗患者住院死亡率的基线呼吸机参数。

结论

由于 ECMO 前 MV 的持续时间与成人呼吸 ECMO 的结果密切相关,建议医疗中心寻找合适的预后工具,以确定具有不同 MV 持续时间的患者开始呼吸 ECMO 的起点。

临床试验注册号

本研究报告了一项针对人类参与者的医疗干预措施,并进行了回顾性注册。2016 年 11 月 23 日,长庚医疗基金会机构审查委员会批准了该研究(编号 201601483B0)。所有数据均于 2016 年 12 月 1 日至 2017 年 1 月 31 日提取。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8c60/5723060/ace1427201c3/12890_2017_520_Fig1_HTML.jpg

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