TY - JOUR T1 - Controlled mechanical ventilation in septic animals: Effects on diaphragm function JF - European Respiratory Journal JO - Eur Respir J VL - 42 IS - Suppl 57 SP - 388 AU - Karen Maes AU - Debby Thomas AU - Cielen Nele AU - Smuder Asley AU - Powers Scott AU - Hermans Greet AU - Stamiris Angela AU - Sabah Hussain AU - Marc Decramer AU - Ghislaine Gayan-Ramirez Y1 - 2013/09/01 UR - http://erj.ersjournals.com/content/42/Suppl_57/388.abstract N2 - Controlled mechanical ventilation (CMV) was shown to result in diaphragmatic dysfunction and atrophy in healthy animals. Whether mechanical ventilation results in more severe diaphragm dysfunction in animals with already weakened diaphragms is not known and was examined in septic animals. Male Wistar rats were either treated with lipopolysaccharide (5 mg/kg) to induce sepsis or with saline. After 12 hours they were divided into 3 groups: sepsis, sepsis+12hCMV and saline+12hCMV. The levels of IL-6 in plasma and in diaphragm were significantly increased in the sepsis+12hCMV group compared to the other groups. Diaphragm force was significantly lower in septic animals compared to saline+12hCMV with an additional decrease in the sepsis+12hCMV group compared to the sepsis group. mRNA expression of diaphragm MuRF1 and atrogin-1, markers of the proteasome system, were significantly higher in the sepsis+12hCMV group compared to the other groups. Diaphragm fiber dimensions and 4-HNE, a marker of oxidative stress, were similar in all groups. LC3B protein lipidation, used as an indirect assessment of autophagy, was increased in sepsis+12hCMV compared to the other groups. Similarly, protein levels of several autophagy-related genes including those involved in the initiation of autophagosome formation (ULK1, BECLIN1, PI3KC3), and targeting of the mitochondria by autophagosomes (SQSTM1, BNIP3 and PARKIN) were significantly increased in sepsis+12hCMV compared to the others. These data clearly show that CMV in septic animals further compromises diaphragm function, activates atrophic pathway and favors autophagosome formation.Supported by FWO-Flanders G.0893.11 and AstraZeneca Pharmaceuticals. ER -