Evolution of gene expression changes in newborn rats after mechanical ventilation with reversible intubation

Mechanical ventilation (MV) is life-saving but potentially harmful for lungs of premature infants. So far, animal models dealt with the acute impact of MV on immature lungs, but less with its delayed effects. We used a newborn rodent model including non-surgical and therefore reversible intubation with moderate ventilation and hypothesized that there might be distinct gene expression patterns after a ventilation-free recovery period compared to acute effects directly after MV. Newborn rat pups were subjected to 8?hr of MV with 60% oxygen (O2), 24?hr after injection of lipopolysaccharide (LPS), intended to create a low inflammatory background as often recognized in preterm infants. Animals were separated in controls (CTRL), LPS injection (LPS), or full intervention with LPS and MV with 60% O2 (LPS?+?MV?+?O2). Lungs were recovered either directly following (T:0?hr) or 48?hr after MV (T:48?hr). Histologically, signs of ventilator-induced lung injury (VILI) were observed in LPS?+?MV?+?O2 lungs at T:0?hr, while changes appeared similar to those known from patients with chronic lung disease (CLD) with fewer albeit larger gas exchange units, at T:48?hr. At T:0?hr, LPS?+?MV?+?O2 increased gene expression of pro-inflammatory MIP-2. In parallel anti-inflammatory IL-1Ra gene expression was increased in LPS and LPS?+?MV?+?O2 groups. At T:48?hr, pro- and anti-inflammatory genes had returned to their basal expression. MMP-2 gene expression was decreased in LPS and LPS?+?MV?+?O2 groups at T:0?hr, but no longer at T:48?hr. MMP-9 gene expression levels were unchanged directly after MV. However, at T:48?hr, gene and protein expression increased in LPS?+?MV?+?O2 group. In conclusion, this study demonstrates the feasibility of delayed outcome measurements after a ventilation-free period in newborn rats and may help to further understand the time-course of molecular changes following MV. The differences obtained from the two time points could be interpreted as an initial transitory increase of inflammation and a delayed impact of the intervention on structure-related genes. Pediatr Pulmonol. 2012; 47:12041214. (C) 2012 Wiley Periodicals, Inc.