Expiratory flow-limitation in mechanically ventilated patients: A risk for ventilator-induced lung injury?

Expiratory flow limitation(EFL), that is the inability of expiratory flow to increase in spite of an increase of the driving pressure, is a common and unrecognized occurrence during mechanical ventilation in a variety of intensive care unit conditions. Recent evidence suggests that the presence of EFL is associated with an increase in mortality, at least in acute respiratory distress syndrome(ARDS) patients, and in pulmonary complications in patients undergoing surgery. EFL is a major cause of intrinsic positive end-expiratory pressure(PEEPi), which in ARDS patients is heterogeneously distributed, with a consequent increase of ventilation/perfusion mismatch and reduction of arterial oxygenation. Airway collapse is frequently concomitant to the presence of EFL.When airways close and reopen during tidal ventilation, abnormally high stresses are generated that can damage the bronchiolar epithelium and uncouple small airways from the alveolar septa, possibly generating the small airways abnormalities detected at autopsy in ARDS. Finally, the high stresses and airway distortion generated downstream the choke points may contribute to parenchymal injury, but this possibility is still unproven. PEEP application can abolish EFL, decrease PEEPi heterogeneity, and limit recruitment/derecruitment.Whether increasing PEEP up to EFL disappearance is a useful criterion for PEEP titration can only be determined by future studies.

Effects of dynamic ventilatory factors on ventilatorinduced lung injury in acute respiratory distress syndrome dogs

BACKGROUND:Mechanical ventilation is a double-edged sword to acute respiratory distress syndrome(ARDS) including lung injury,and systemic inflammatory response high tidal volumes are thought to increase mortality.The objective of this study is to evaluate the effects of dynamic ventilatory factors on ventilator induced lung injury in a dog model of ARDS induced by hydrochloric acid instillation under volume controlled ventilation and to investigate the relationship between the dynamic factors and ventilator-induced lung injuries(VILI) and to explore its potential mechanisms.METHODS:Thirty-six healthy dogs were randomly divided into a control group and an experimental group.Subjects in the experimental group were then further divided into four groups by different inspiratory stages of flow.Two mL of alveolar fluid was aspirated for detection of IL-8 and TNF-α.Lung tissue specimens were also extracted for total RNA,IL-8 by western blot and observed under an electronic microscope.RESULTS:IL-8 protein expression was significantly higher in group B than in groups A and D.Although the IL-8 protein expression was decreased in group C compared with group B,the difference was not statistically significant.The TNF-α ray degree of group B was significantly higher than that in the other groups(P<0.01),especially in group C(P>0.05).The alveolar volume of subjects in group B was significantly smaller,and cavity infiltration and cell autolysis were marked with a significant thicker alveolar septa,disorder of interval structures,and blurring of collagenous and elastic fiber structures.A large number of necrotic debris tissue was observed in group B.CONCLUSION:Mechanical ventilation with a large tidal volume,a high inspiratory flow and a high ventilation frequency can cause significant damage to lung tissue structure.It can significantly increase the expression of TNF-α and IL-8 as well as their mRNA expression.Furthermore,the results of our study showed that small tidal ventilation significantly reduces the release of proinflammatory media.This finding suggests that greater deterioration in lung injury during ARDS is associated with high inspiratory flow and high ventilation rate.

Rho/Rock信号通路在大鼠呼吸机相关性肺损伤中的作用

目的评价Rho/Rock信号通路在大鼠呼吸机相关性肺损伤（ventilator-induced lung injury,VILI）中的作用。方法选择健康雄性SD大鼠96只,12~15周龄,体重300~350g,采用随机数字表法将大鼠随机分为四组：空白对照组（C组）、Rho激酶抑制药法舒地尔组（F组）、高潮气量组（H组）和高潮气量＋Rho激酶抑制药法舒地尔组（HF组）,每组24只。C组和F组不行机械通气,H组和HF组行高潮气量40ml/kg机械通气4h。F组和HF组在机械通气前1h给予腹腔注射法舒地尔10mg/kg。分别于通气前（T0）、通气后4h（T1）、8h（T2）和24h（T3）每组随机取6只大鼠,采集血样,测定血清TNF-α、IL-6及IL-10浓度;采血结束后处死大鼠,收集支气管肺泡灌洗液（BALF）,采用考马斯亮兰法检测BALF总蛋白;测定肺组织湿/干重比（W/D）;光镜下行肺组织病理学损伤评分;采用分光光度法检测肺组织髓过氧化物酶（MPO）活性;采用Western blot和RT-PCR法分别检测肺组织RhoA、Rock2蛋白含量和mRNA表达水平。结果与C组比较,T1~T3时H组和HF组大鼠血清TNF-α、IL-6及IL-10浓度、BALF总蛋白含量、肺组织W/D、病理学损伤评分、MPO活性、RhoA、Rock2蛋白含量和mRNA表达水平明显升高（P〈0.05）;与H组比较,T1~T3时HF组大鼠血清TNF-α、IL-6浓度、BALF总蛋白含量、肺组织W/D、病理学损伤评分、MPO活性、RhoA、Rock2蛋白含量和mRNA表达水平明显下降,血清IL-10浓度明显升高（P〈0.05）。结论Rho激酶抑制药法舒地尔可减轻大鼠呼吸机相关性肺损伤,其机制可能与其抑制Rho/Rock信号通路,降低肺组织内炎性反应有关。

基于络病学探讨内毒素“二次打击”急性肺损伤大鼠的Rho/ROCK机制及川芎嗪的保护作用

目的:研究内毒素血症"瘀滞络脉"急性肺损伤大鼠的Rho/ROCK机制及川芎嗪的保护作用。方法:以内毒素"二次打击"建立大鼠内毒素血症"瘀滞络脉"急性肺损伤模型,分别设正常对照组、模型组、川芎嗪低剂量组、高剂量组,测定呼吸频率、肺泡灌洗液中性粒细胞(PMN)百分率、肺湿/干重比、肺组织髓过氧化物酶(Myeloperoxidase,MPO)活性、ROCK mRNA表达量,并观察、评估肺组织损伤严重程度。结果:与模型组相比,川芎嗪显著降低呼吸频率、PMN百分率、肺湿/干重比、MPO活性、ROCK mRNA表达量,减轻大鼠急性肺损伤病理改变。结论:川芎嗪可能通过抑制Rho/ROCK通路对内毒素血症"瘀滞络脉"大鼠急性肺损伤有较好的保护作用。

右美托咪定减轻呼吸机相关性肺损伤模型大鼠肺组织损伤

目的探讨右美托咪定(DEX)对呼吸机相关性肺损伤(VILI)大鼠肺组织Ras同源基因家族成员A(RhoA)/Rho激酶1(ROCK1)信号通路的影响。方法建立VILI大鼠模型,将大鼠分为对照组(control组)、模型组(VILI组)、右美托咪定低、高剂量组(DEX-L、DEX-H组)、右美托咪定高剂量+溶血磷脂酸(LPA)组(DEX-H+LPA组)。测定大鼠肺组织湿/干质量比值(W/D);HE染色观察肺组织病理形态;ELISA试剂盒检测支气管肺泡灌洗液(BALF)中肿瘤坏死因子α(TNF-α)、白细胞介素-1β(IL-1β)、白细胞介素-6(IL-6)的水平;TUNEL染色法检测肺上皮细胞死亡;Western blot检测细胞凋亡相关蛋白及RhoA、ROCK1表达水平。结果DEX可以减轻VILI大鼠肺损伤,降低肺损伤评分、W/D、细胞凋亡率和TNF-α、IL-1β、IL-6水平及Bax、cleaved caspase-3、RhoA、ROCK、α-SMA表达(P<0.05),升高Bcl-2表达(P<0.05);LPA可以促使大鼠肺损伤加重,肺损伤评分、W/D、细胞凋亡率和TNF-α、IL-1β、IL-6水平及Bax、cleaved caspase-3、RhoA、ROCK、α-SMA表达升高(P<0.05),Bcl-2表达降低(P<0.05)。结论右美托咪定可能通过抑制RhoA/ROCK1通路保护大鼠呼吸机相关性肺损伤。

Driving pressure decoded:Precision strategies in adult respiratory distress syndrome management

Mechanical ventilation(MV)is an important strategy for improving the survival of patients with respiratory failure.However,MV is associated with aggravation of lung injury,with ventilator-induced lung injury(VILI)becoming a major concern.Thus,ventilation protection strategies have been developed to minimize complications from MV,with the goal of relieving excessive breathing workload,improving gas exchange,and minimizing VILI.By opting for lower tidal volumes,clinicians seek to strike a balance between providing adequate ventilation to support gas exchange and preventing overdistension of the alveoli,which can contribute to lung injury.Additionally,other factors play a role in optimizing lung protection during MV,including adequate positive end-expiratory pressure levels,to maintain alveolar recruitment and prevent atelectasis as well as careful consideration of plateau pressures to avoid excessive stress on the lung parenchyma.

异丙酚通过Rho/Rock信号通路调控大鼠呼吸机相关性肺损伤的机制研究

目的探讨异丙酚通过Rho/Rock信号通路调控大鼠呼吸机相关性肺损伤的机制。方法 40只成年雄性SD大鼠随机分为4组,每组10只,分别为双肺通气组(TLV组),单肺通气组(OLV足),单肺通气+异丙酚组(D组),单肺通气+异丙酚+法舒地尔组(DL组)。对各组大鼠血清血清TNF-α、IL-6及IL-10含量及肺组织RhoA及Rock2蛋白水平和基因表达水平进行测定。结果 D组和DL组大鼠血清TNF-α、IL-6水平低于TLV和OLV组,IL-10水平高于TLV和OLV组,差异有统计学意义(P<0.05)。DL组血清TNF-α、IL-6水平低于D组,IL-10水平高于D组,差异有统计学意义(P<0.05)。D组和DL组大鼠W/D及BALF总蛋白水平低于TLV和OLV组,差异有统计学意义(P<0.05)。D组和DL组大鼠RhoA和Rock2蛋白含量低于TLV和OLV组,差异有统计学意义(P<0.05)。DL组大鼠RhoA和Rock2蛋白含量水平低于D组,差异有统计学意义(P<0.05)。结论异丙酚能够有效缓解呼吸机相关肺损伤的炎性反应,同时其作用机制可能与其能够抑制Rho/Rock信号通路的激活有关。

Rho/Rho激酶信号通路与急性肺损伤/急性呼吸窘迫综合征

Rho/Rho激酶信号通路参与调节细胞的收缩、黏附、迁移、增殖、凋亡等多种生物学行为和功能,随着对Rho/Rho激酶信号通路研究的深入,发现其在急性肺损伤/急性呼吸窘迫综合征中发挥着重要的作用。笔者就Rho/Rho激酶信号通路在急性肺损伤/急性呼吸窘迫综合征中的作用机制作一综述。

乌司他丁通过Rho／ROCK信号通路改善脂多糖诱导脓毒症小鼠肺损伤的研究

目的探讨乌司他丁（UTI）对脂多糖（LPS）诱导脓毒症小鼠肺损伤的保护作用及其分子机制。方法将C57BL／6小鼠随机分为对照组（Con组，n=10）、模型组（LPS组，n=10）及UTI干预组（L＋U组，n=30），建立LPS脓毒症小鼠模型。采用肺湿干质量（W／D）法及伊文思蓝（EvansBlue，EB）法观察各组小鼠肺组织含水量及肺微血管通透性的变化，HE染色法检测各组小鼠肺组织病理变化，免疫组化法检测肺组织血管钙黏蛋白（VE-cadherin）及ROCK2的表达。结果与Con组比较，LPS组小鼠肺组织W／D及EB含量均明显增加（均P〈0．05），而L＋U组W／D及EB含量明显降低，其中UTI在10^4U／kg、10^5U／kg剂量时，与LPS组比较差异有统计学意义（均P〈0．05）；LPS组小鼠较Con组肺组织损伤严重，L＋U组肺组织损伤明显减轻；免疫组化结果显示，LPS组小鼠肺组织VE—cadherin表达明显降低，ROCK2表达明显增高（均P〈0．05），而UTI干预后，VE—cadherin表达明显增加，ROCK表达明显下降（均P〈0．05）。结论UTI能够剂量依赖性地降低LPS所致的肺毛细血管通透性增加，从而改善脓毒症小鼠肺损伤，这一作用可能与UTI抑制Rho／ROCK信号通路的激活有关。

Molecular Mechanisms of Ventilator-Induced Lung Injury

Objective：Mechanical ventilation （MV） has long been used as a life-sustaining approach for several decades.However,researchers realized that MV not only brings benefits to patients but also cause lung injury if used improperly,which is termed as ventilator-induced lung injury （VILI）.This review aimed to discuss the pathogenesis of VILI and the underlying molecular mechanisms.Data Sources：This review was based on articles in the PubMed database up to December 2017 using the following keywords：＂ventilator-induced lung injury＂,＂pathogenesis＂,＂mechanism＂,and ＂biotrauma＂.Study Selection：Original articles and reviews pertaining to mechanisms of VILI were included and reviewed.Results：The pathogenesis of VILI was defined gradually,from traditional pathological mechanisms （barotrauma,volutrauma,and atelectrauma） to biotrauma.High airway pressure and transpulmonary pressure or cyclic opening and collapse of alveoli were thought to be the mechanisms of barotraumas,volutrauma,and atelectrauma.In the past two decades,accumulating evidence have addressed the importance of biotrauma during VILI,the molecular mechanism underlying biotrauma included but not limited to proinflammatory cytokines release,reactive oxygen species production,complement activation as well as mechanotransduction.Conclusions：Barotrauma,volutrauma,atelectrauma,and biotrauma contribute to VILI,and the molecular mechanisms are being clarified gradually.More studies are warranted to figure out how to minimize lung injury induced by MV.

Serum and lung endothelin-1 increased in a canine model of ventilator-induced lung injury

Background Nitric oxide （NO） plays an important role in acute lung injury （ALl）, acute respiratory distress syndrome （ARDS）, and in ventilator-induced lung injury （VILI）. A change in the balance of endothelin-1 （ET-1） and NO in the ALI/ARDS can also add to these problems. However, the profile of ET-1 and the balance of ET-1 and NO are still unknown in a VILI model. Methods Models of oleic acid induced ALl were established in dogs; these models were then randomized into three groups undergone different tidal volume （VT） mechanical ventilation, which included a VT6 group （VT equaled to 6 ml/kg body weight, positive end expiratory pressure （PEEP） equaled to 10 cmH20, n=-6）, a VT10 group （VT equaled to 10 ml/kg body weight, PEEP equaled to 10 cmH20, n=-4） and a VT20 group （VT equaled to 20 ml/kg body weight, PEEP equaled to 10 cmH20, n=-6） for 6-hour ventilation. The levels of ET-1 and NO in serum and tissue homogenates of lung were observed throughout the trial. Results PaO2 was increased after mechanical ventilation, but hypercapnia occurred in the VT6 group. The magnitudes of lung injury in the VT20 group were more severe than those in the VT6 group and the VT10 group. Serum levels of ET-1 and NO increased after ALl models were established and slightly decreased after a 6-hour ventilation in both the VT6 group and the VT20 group. The serum ET-1 level in the VT20 group was higher than that in the VT6 group and the VT10 group after the 6-hour ventilation （P 〈0.05） while the serum NO levels were similar in the three groups （all P 〉0.05）. There was no significant difference in serum ratio of ET-1/NO between any two out of three groups （P 〉0.05）, although there was a significant positive relationship between serum ET-1 and serum NO （r=0.80, P 〈0.01）. The levels of ET-1 and NO in the lung were increased after ventilation. The lung ET-1 level in the VT20 group was significantly higher than that in the VT6 group and VT10 group （both P 〈0.05） while there was no significant difference in lung NO levels between two groups （P〉0.05）. In the lung tissue, the ratio of ET-1/NO was significantly higher in the VT20 group than in the VT6 group and VT10 group after the 6-hour ventilation （P 〈0.05） as there was a significant positive relationship between ET-1 and NO in the lung （r=0.54, P 〈0.05）. Conclusions The production of ET-1 and NO was increased in serum and lung tissue in a VILI model. But the ET-1 levels increased much more than the NO levels in the lung, though there was a significant positive relationship between levels of ET-1 and NO. These results showed that there was an interaction between ET-1 and NO in a VILI model and changing the balance of ET-1 and NO levels might contribute to the pathophysiologic process of VILI.

Mesenchymal Stem Cell Attenuates Neutrophil-predominant Inflammation and Acute Lung Injury in an In Vivo Rat Model of Ventilator-induced Lung Injury

Background： Subsequent neutrophil （polymorphonuclear neutrophil [PMN]）-predominant inflammatory response is a predominant feature of ventilator-induced lung injury （VILI）, and mesenchymal stem cell （MSC） can improve mice survival model of endotoxin-induced acute lung injury, reduce lung impairs, and enhance the repair inflammatory in the VILI is still unknown. This study aimed to inflammatory in the mechanical VILI. of VILI. However, whether MSC could attenuate PMN-predominant test whether MSC intervention could attenuate the PMN-predominate Methods： Sprague-Dawley rats were ventilated for 2 hours with large tidal volume （20 mL/kg）. MSCs were given before or after ventilation. The inflammatory chemokines and gas exchange were observed and compared dynamically until 4 hours after ventilation, and pulmonary pathological change and activation of PMN were observed and compared 4 hours after ventilation. Results： Mechanical ventilation （MV） caused significant lung injury reflected by increasing in PMN pulmonary sequestration, inflammatory chemokines （tumor necrosis factor-alpha, interleukin-6 and macrophage inflammatory protein 2） in the bronchoalveolar lavage fluid, and injury score of the lung tissue. These changes were accompanied with excessive PMN activation which reflected by increases in PMN elastase activity, production of radical oxygen series. MSC intervention especially pretreatment attenuated subsequent lung injury, systemic inflammation response and PMN pulmonary sequestration and excessive PMN activation initiated by injurious ventilation. Conclusions： MV causes profound lung injury and PMN-predominate inflammatory responses. The protection effect of MSC in the VILI rat model is related to the suppression of the PMN activation.

Respiratory mechanics in brain injury: A review

Several clinical and experimental studies have shown that lung injury occurs shortly after brain damage. The responsible mechanisms involve neurogenic pulmonary edema, inflammation, the harmful action of neurotransmitters, or autonomic system dysfunction. Mechanical ventilation, an essential component of life support in brain-damaged patients(BD), may be an additional traumatic factor to the already injured or susceptible to injury lungs of these patients thus worsening lung injury, in case that non lung protective ventilator settings are applied. Measurement of respiratory mechanics in BD patients, as well as assessment of their evolution during mechanical ventilation, may lead to preclinical lung injury detection early enough, allowing thus the selection of the appropriate ventilator settings to avoid ventilatorinduced lung injury. The aim of this review is to explore the mechanical properties of the respiratory system in BD patients along with the underlying mechanisms, and to translate the evidence of animal and clinical studies into therapeutic implications regarding the mechanical ventilation of these critically ill patients.

Rho激酶抑制剂在大鼠肺缺血再灌注损伤中的保护作用的研究

目的探讨Rho激酶抑制剂盐酸法舒地尔在大鼠肺缺血再灌注损伤中的保护作用及机制。方法将24只大鼠随机分为3组,假手术组(sham组)、缺血再灌注组(IR组)、缺血再灌注+Rho激酶抑制剂组,缺血1小时再灌注2小时后,获取左肺标本,对三组肺组织进行病理检查,同时检测三组肺组织湿干重比、肺组织肿瘤坏死因子(TNF-α)/白细胞介素(IL-6)、髓过氧化物酶(myeloperoxidase,MPO)的水平。结果经Rho激酶抑制剂预处理后的肺组织病理损伤较IR组轻,同时肺组织湿干重比、TNF-α/IL-6、MPO的水平也较IR组低,所有差异均有统计学意义,P<0.05。结论 Rho激酶抑制剂通过减少炎性细胞因子的表达及氧自由基的产生在肺缺血再灌注损伤中发挥保护作用。

Experimental study on the protective effect of ulinastatin on lung tissue in rats with severe scalded

Objective:To explore the potential protective effects of ulinastatin on ventilation-induced lung injuries of severe burned rats.Methods:Ninety Wistar rats were randomly divided into three experimental groups:the control group(n=30),the ventilation group(n=30)and the ventilation-ulinastatin group(n=30).After establishing the severe burn model,the rats of latter two groups were mechanically ventilated for 1 hour with or without the pre-treatment of ulinastatin.After severe scald,the protective effect of ulinastatin on lung injury caused by mechanical ventilation was estimated through the observation of the tissues samples,and evaluation of the pathological changes of lung tissue by HE staining,ultrastructure change by electron microscopy,lung coefficient,and the expression levels of lung tissue cytokines TNF-α,IFN-γ,IL-2 by immunohistochemical staining.Results:Edema in lung tissues of the control group and the ventilation group was obvious,the hemorrhagic focus could be seen,and the cut surface was observed to be scattered and swelling;Edema in lung tissues of the ventilation-ulinastatin group was mild.HE staining revealed that the pathological changes of the ventilation-ulinastatin group were milder than the ventilation group.Under the electron microscope,the lung tissue organelles of the control group and the ventilation group were seriously damaged;the corresponding changes in the ventilation-ulinastatin group were lighter.The lung coefficient of the ventilation-ulinastatin group was significantly lower than that in the ventilation group.The immunohistochemical results showed that the intensity of TNF-α,IL-2 and IFN-γin lung tissue of the ventilation-ulinastatin group was significantly lower than that in the ventilation group.Conclusions:Ulinastatin has protective effects on lung injury caused by mechanical ventilation in severe scalded rats,whose mechanism may be related to the capacity of ulinastatin to reduce the expression of cytokines including TNF-α,IL-2 and IFN-γ.

高氧致SD大鼠年龄相关的肺损伤及可能机制

目的·观察新生鼠和幼鼠高氧肺损伤的异同,并初步探索Rho/Rock信号通路在年龄相关高氧肺损伤中的作用。方法·将新生SD大鼠(新生鼠)与3周龄SD大鼠(幼鼠)分为新生鼠空气组、新生鼠高氧组、幼鼠空气组、幼鼠高氧组,建立动物模型直至第14日,统计生存率、体质量变化,取SD大鼠肺组织行病理学检查、损伤程度评分、羟脯氨酸含量测定、SOD与MDA检测,以及ROCK1、p-MYPT1、MYPT1表达的检测。结果·①新生鼠高氧组较新生鼠空气组、幼鼠空气组、幼鼠高氧组生存率明显降低,幼鼠空气组与高氧组生存率无明显差异;新生鼠高氧组较空气组、幼鼠高氧组较空气组体质量增长缓慢,且新生鼠高氧组较幼鼠高氧组体质量增长更为缓慢。②新生鼠高氧组、幼鼠高氧组出现啼组织损伤及纤维化改变,且新生鼠较幼鼠更为严重。③新生鼠高氧组较空气组、幼鼠高氧组较空气组MDA含量升高,SOD活力降低;与幼鼠高氧组相比,新生鼠高氧组SOD活力基础值较低且高氧后降低更为明显。④新生鼠高氧组较空气组、幼鼠高氧组较空气组肺组织ROCK1蛋白表达有上升趋势,p-MYPT1蛋白表达增强,且新生鼠高氧组较幼鼠高氧组p-MYPT1蛋白表达增强更为明显。结论·高氧肺损伤具有年龄依赖性,新生鼠对高氧耐受力明显弱于幼鼠,与其自身抗氧化能力弱有关;Rho/Rock信号通路活化程度的不同可能在年龄相关高氧肺损伤中发挥重要作用。

法舒地尔对脂多糖诱导的大鼠急性肺损伤的影响

目的：探讨法舒地尔通过RhoA/ROCK（ Rho激酶）通路是否能减轻脂多糖（ LPS）诱导的大鼠急性肺损伤（ ALI）。方法：18只Wistar健康大鼠随机分为对照组（ NS组）、脂多糖组（ LPS组）及法舒地尔干预组（ FAS组）各6只；LPS组和FAS组采用小剂量LPS 1 mg/kg腹腔注射16 h后,气管内滴注LPS 3 mg/kg建立ALI模型。 FAS组在腹腔注射LPS前30 min和气管滴注LPS后1 h给予腹腔注射法舒地尔10 mg/kg。于气管滴注LPS造模后,观察3 h后处死大鼠,通过HE染色观察各组肺组织形态学改变,测肺组织湿/干重比、丙二醛含量、髓过氧化物酶活性,反转录-聚合酶链反应及Western blot法检测肺组织匀浆中ROCK2（Rho激酶2）mRNA及蛋白的表达情况。结果：与NS组比较,LPS组肺组织病理形态学改变明显,FAS组较LPS组相比明显减轻；LPS组肺湿/干重比、丙二醛含量和髓过氧化物酶活性均较NS组明显增高（P〈0.01）,而FAS组较LPS组均有不同程度降低（P〈0.05-P〈0.01）；LPS组ROCK2 mRNA 表达较NS组明显增高（P〈0.01）,而FAS组与LPS组差异无统计学意义（P〉0.05）；LPS组ROCK2蛋白表达较NS组明显增高（P〈0.01）,而FAS组较LPS组表达水平降低（P〈0.05）。结论：法舒地尔通过RhoA/Rho激酶信号通路能够减轻LPS诱导的大鼠ALI。

地塞米松和法舒地尔对油酸致小鼠急性肺损伤伤情的影响

目的探讨地塞米松和法舒地尔(fasudil)对油酸致小鼠急性肺损伤的影响及ROCK(Rho-associated coiledcoil forming kinase)在其中的作用。方法采用油酸致C57小鼠急性肺损伤模型,观察伤后24h各组肺组织病理及肺含水率、ROCK活性、ROCK1和ROCK2蛋白含量及IL-1βmRNA的变化。结果地塞米松和法舒地尔均可显著减轻油酸肺组织中炎性细胞浸润、肺出血等病理变化,降低肺含水率(P<0.05),抑制肺组织ROCK活性(P<0.05),降低IL-1βmRNA的表达水平;地塞米松对ROCK1的表达水平无影响,但可增强ROCK2的表达,法舒地尔对ROCK1和ROCK2的表达水平均无影响。结论地塞米松和法舒地尔均可通过抑制肺组织内炎性细胞浸润明显减轻油酸引起的急性肺损伤,而地塞米松的治疗作用可能与对其ROCK活性的抑制有关。

百令胶囊对急性胰腺炎模型大鼠肺损伤的修复作用

目的探讨百令胶囊对急性胰腺炎模型大鼠肺损伤的修复作用。方法将72只Wistar大鼠随机分为假手术组(等体积生理盐水灌胃),模型组(等体积生理盐水灌胃),百令胶囊低、中、高剂量组(1,2,4 g/kg灌胃)及法舒地尔组(30 mg/kg腹腔注射),各12只。除假手术组外,其余5组大鼠均胰胆管注射4%牛磺胆酸钠(1 mL/kg)以复制胰腺炎大鼠模型,建模成功后,各组大鼠均予相应药物或生理盐水,每天1次,连续5 d。采用酶联免疫吸附(ELISA)法测定大鼠血清淀粉酶、白细胞介素6(IL-6)、肿瘤坏死因子-α(TNF-α)及肺组织髓过氧化物酶(MPO)、超氧化物歧化酶(SOD)、活性氧(ROS)水平;采用血气分析仪测定二氧化碳分压(PaCO_(2))、氧分压(PaO_(2)),并计算氧合指数(OI);称定大鼠肺组织湿质量(W)及干质量(D)并计算W/D;采用苏木素-伊红(HE)染色,检查肺组织病理形态学;采用实时定量聚合酶链式反应法及Westernblot法分别测定RhoA、Rho激酶1(ROCK1)、Rho激酶2(ROCK2)mRNA及蛋白表达水平。结果与模型组比较,百令胶囊低、中、高剂量组及法舒地尔组大鼠的血清淀粉酶及IL-6,TNF-α,PaCO_(2),MPO,ROS水平,肺组织W/D及RhoA,ROCK1,ROCK2 mRNA和蛋白水平均显著降低(P<0.05),PaO_(2),OI,SOD水平均显著升高(P<0.05),大鼠肺组织病理形态学显著改善。结论百令胶囊能改善急性胰腺炎肺损伤模型大鼠的肺功能,其机制可能与抑制Rho/ROCK通路,继而抑制炎性因子释放及氧化损伤有关。

Efficacy of prone position in acute respiratory distress syndrome patients: A pathophysiology-based review

Acute respiratory distress syndrome(ARDS) is a syndrome with heterogeneous underlying pathological processes. It represents a common clinical problem in intensive care unit patients and it is characterized by high mortality. The mainstay of treatment for ARDS is lung protective ventilation with low tidal volumes and positive end-expiratory pressure sufficient for alveolar recruitment. Prone positioning is a supplementary strategy available in managing patients with ARDS. It was first described 40 years ago and it proves to be in alignment with two major ARDS pathophysiological lung models; the "sponge lung"- and the "shape matching"-model. Current evidence strongly supports that prone positioning has beneficial effects on gas exchange, respiratory mechanics, lung protection and hemodynamics as it redistributes transpulmonary pressure, stress and strain throughout the lung and unloads the right ventricle. The factors that individually influence the time course of alveolar recruitment and the improvement in oxygenation during prone positioning have not been well characterized. Although patients' response to prone positioning is quite variable and hard to predict, large randomized trials and recent meta-analyses show that prone position in conjunction with a lung-protective strategy, when performed early and in sufficient duration, may improve survival in patients with ARDS. This pathophysiology-based review and recent clinical evidence strongly support the use of prone positioning in the early management of severe ARDS systematically and not as a rescue maneuver or a last-ditch effort.