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首页> 外文期刊>Resuscitation. >Ventilator-induced lung injury (VILI) promotes ischemia/reperfusion lung injury (I/R) and NF-kappaB antibody attenuates both injuries.
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Ventilator-induced lung injury (VILI) promotes ischemia/reperfusion lung injury (I/R) and NF-kappaB antibody attenuates both injuries.

机译:呼吸机诱发的肺损伤(VILI)促进缺血/再灌注性肺损伤(I / R),NF-κB抗体可减轻这两种损伤。

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RATIONALE: Whether the ventilator-induced lung injury (VILI) superimposed on ischemia/reperfusion injury (I/R) causes synergistic damage has not been well explored. Whether nuclear factor-kappa B (NF-kappaB) antibody has protective effects for both injuries is also unknown. METHODS: I/R and VILI were produced in an isolated rat lung model. Hemodynamics, lung weight gain (LWG), capillary filtration coefficient (K(fc)), cytokines, and lung pathology were assessed. RESULTS: VILI or I/R produced similar permeability pulmonary edema which was reflected by increasing K(fc) and LWG. Cytokine (IL-1beta) up-regulation occurred in both injuries. Pathologic examination showed edema and inflammatory cell infiltration in VILI or I/R. In addition, the alveoli were overdistended and even ruptured because of marked inhomogeneity of inflation in VILI. Furthermore, combined I/R and VILI produced further increases in K(fc), LWG, IL-1beta, as well as more severe pathologic changes. Conversely, less permeability pulmonary edema, pathologic changes and IL-1 expression were found in groups pretreated with anti-NF-kappaB antibody. CONCLUSION: VILI and I/R cause synergistic damage on the lung. I/R or VILI alone or combined can be attenuated by NF-kappaB antibody. NF-kappaB plays an important role in both forms of lung injury. We propose anti-NF-kappaB antibody pretreatment to be beneficial for VILI, I/R and lung transplantation.
机译:理由:呼吸机诱发的肺损伤(VILI)与缺血/再灌注损伤(I / R)叠加是否会引起协同损伤尚未得到很好的研究。还不清楚核因子-κB(NF-kappaB)抗体是否对两种损伤都有保护作用。方法:I / R和VILI在分离的大鼠肺模型中产生。评估了血流动力学,肺增重(LWG),毛细血管滤过系数(K(fc)),细胞因子和肺病理学。结果:VILI或I / R产生相似的通透性肺水肿,这通过增加K(fc)和LWG反映出来。两种损伤均发生细胞因子(IL-1beta)上调。病理检查显示VILI或I / R中有水肿和炎性细胞浸润。此外,由于VILI的通气明显不均匀,肺泡过度扩张甚至破裂。此外,组合的I / R和VILI会进一步增加K(fc),LWG,IL-1beta,以及更严重的病理变化。相反,在用抗NF-κB抗体预处理的组中发现通透性较低的肺水肿,病理变化和IL-1表达。结论:VILI和I / R对肺造成协同损害。单独或联合使用的I / R或VILI可被NF-κB抗体减弱。 NF-κB在两种形式的肺损伤中都起着重要作用。我们建议抗NF-κB抗体预处理对VILI,I / R和肺移植有益。

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