Gene expression of important components involved in lung remodeling process in ventilator induced lung injury

INTRODUCTION: In spite of being essential, in some situations mechanical ventilation (MV) can lead to damages to the lung, an event known as ventilator-induced lung injury. This process depends on the action of mechanical forces and lung inflammatory response. OBJECTIVE: Analyze lung inflammation and gene expression of proteoglycans and cytoskeleton proteins in response to two mechanisms of VILI (high volume and high pressure). METHODS: Twenty-one rabbits were randomized into three groups: Control, n=6; VT=8ml/kg, PEEP=5 cm H2O, flow = 2l/min; High volume (HV), n=7; VT=16 ml/kg, PEEP 5 cm H2O, flow = 3 l/min and High pressure (HP), n=8; with maximal inspiratory pressure (PIMAX) of 30cmH2O and PEEP 12cmH2O, with the intention of maintaining the same tidal volume as the LV group.. Animals were ventilated for 3h30m and subsequently exsanguinated. RESULTS: There was a reduction in lung compliance in the HP group when compared to control (p=.001) and HV groups (p=.000). Histological analysis did not show difference in inflammatory cells infiltrate between groups, in the same way, no differences in interleukin 8 gene expression were observed. Alpha-actin gene expression did not show any statistical differences between groups. Differences in proteoglycan expression between lung regions were only noticed in the HV group, with Biglycan (p=.004) and lumican (p=.003) gene expression increased in the non-dependent region. Comparisons between groups concerning the nondependent region showed increased expression of biglycan in HP versus control (p=.005). Comparisons between groups addressing the dependent region showed increased expression of decorin in HP (p=.049) and increased expression of versican in HV (p=.003) and HP (p=.015) versus control; and the HP group showed the highest Biglycan (p=.007) and lumican (p=.021) expressions. CONCLUSION: The forces generated by MV act on the lung parenchyma determining alterations in the gene expression of the proteoglycans, independently of the inflammatory response. Pressure and volume act in different ways, being alterations of force imposed by high volumes, felt more by the non-dependent lung regions. The high transpulmonary maintained pressure was the greatest inducer of expression of fibrogenesis related ECM components (AU)