肺部炎症中的碱性磷酸酶——一项针对机械通气危重症患者和大鼠的转化研究
Alkaline phosphatase in pulmonary inflammation-a translational study in ventilated critically ill patients and rats.
作者信息
Juschten Jenny, Ingelse Sarah A, Bos Lieuwe D J, Girbes Armand R J, Juffermans Nicole P, van der Poll Tom, Schultz Marcus J, Tuinman Pieter Roel
机构信息
Department of Intensive Care, Amsterdam University Medical Centers, location "VU", Mail stop ZH 7D-172, De Boelelaan 1117, 1082 RW, Amsterdam, the Netherlands.
Research VUmc Intensive Care (REVIVE), Amsterdam University Medical Centers, location "VU", Amsterdam, the Netherlands.
出版信息
Intensive Care Med Exp. 2020 Dec 18;8(Suppl 1):46. doi: 10.1186/s40635-020-00335-x.
BACKGROUND
Alkaline phosphatase (AP), a dephosphorylating enzyme, is involved in various physiological processes and has been shown to have anti-inflammatory effects.
AIM
To determine the correlation between pulmonary AP activity and markers of inflammation in invasively ventilated critically ill patients with or without acute respiratory distress syndrome (ARDS), and to investigate the effect of administration of recombinant AP on pulmonary inflammation in a well-established lung injury model in rats METHODS: AP activity was determined and compared with levels of various inflammatory mediators in bronchoalveolar lavage fluid (BALF) samples obtained from critically ill patients within 2 days of start of invasive ventilation. The endpoints of this part of the study were the correlations between AP activity and markers of inflammation, i.e., interleukin (IL)-6 levels in BALF. In RccHan Wistar rats, lung injury was induced by intravenous administration of 10 mg/kg lipopolysaccharide, followed by ventilation with a high tidal volume for 4 h. Rats received either an intravenous bolus of 1500 IU/kg recombinant AP or normal saline 2 h after intravenous LPS administration, right before start of ventilation. Endpoints of this part of the study were pulmonary levels of markers of inflammation, including IL-6, and markers of endothelial and epithelial dysfunction.
RESULTS
BALF was collected from 83 patients; 10 patients had mild ARDS, and 15 had moderate to severe ARDS. AP activity correlated well with levels of IL-6 (r = 0.70), as well as with levels of other inflammatory mediators. Pulmonary AP activity between patients with and without ARDS was comparable (0.33 [0.14-1.20] vs 0.55 [0.21-1.42] U/L; p = 0.37). Animals with acute lung injury had markedly elevated pulmonary AP activity compared to healthy controls (2.58 [2.18-3.59] vs 1.01 [0.80-1.46] U/L; p < 0.01). Intravenous administration of recombinant AP did neither affect pulmonary inflammation nor endothelial and epithelial dysfunction.
CONCLUSIONS
In ventilated critically ill patients, pulmonary AP activity correlates well with markers of pulmonary inflammation, such as IL-6 and IL-8. In animals with lung injury, pulmonary AP activity is elevated. Administration of recombinant AP does not alter pulmonary inflammation and endothelial or epithelial dysfunction in the acute phase of a murine lung injury model.
背景
碱性磷酸酶(AP)是一种去磷酸化酶,参与多种生理过程,且已显示具有抗炎作用。
目的
确定有或无急性呼吸窘迫综合征(ARDS)的有创通气危重症患者肺AP活性与炎症标志物之间的相关性,并在已建立的大鼠肺损伤模型中研究重组AP给药对肺部炎症的影响。
方法
在有创通气开始后2天内,测定危重症患者支气管肺泡灌洗液(BALF)样本中的AP活性,并与各种炎症介质水平进行比较。本研究这一部分的终点是AP活性与炎症标志物之间的相关性,即BALF中白细胞介素(IL)-6水平。在RccHan Wistar大鼠中,通过静脉注射10mg/kg脂多糖诱导肺损伤,随后以高潮气量通气4小时。大鼠在静脉注射LPS后2小时,即通气开始前,接受1500IU/kg重组AP静脉推注或生理盐水。本研究这一部分的终点是肺部炎症标志物水平,包括IL-6,以及内皮和上皮功能障碍标志物。
结果
从83例患者中采集了BALF;10例患者患有轻度ARDS,15例患有中度至重度ARDS。AP活性与IL-6水平(r = 0.70)以及其他炎症介质水平密切相关。有ARDS和无ARDS患者的肺AP活性相当(0.33 [0.14 - 1.20] vs 0.55 [0.21 - 1.42] U/L;p = 0.37)。与健康对照相比,急性肺损伤动物的肺AP活性显著升高(2.58 [2.18 - 3.59] vs 1.01 [0.80 - 1.46] U/L;p < 0.01)。静脉注射重组AP既不影响肺部炎症,也不影响内皮和上皮功能障碍。
结论
在有创通气的危重症患者中,肺AP活性与肺部炎症标志物如IL-6和IL-8密切相关。在肺损伤动物中,肺AP活性升高。在小鼠肺损伤模型的急性期,给予重组AP不会改变肺部炎症以及内皮或上皮功能障碍。
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