PPAR?/? agonists are known to modulate the systemic inflammatory response after sepsis. In this study, inflammation modulation effects of PPAR?/? are investigated using the selective PPAR?/? agonist (GW0742) in a model of haemorrhagic shock (HS)-induced sterile systemic inflammation.Blood pressure-controlled (35±5mmHg) HS was performed in C57/BL6 mice for 90min. Low-dose GW0742 (0.03mg/kg/BW) and high-dose GW0742 (0.3mg/kg/BW) were then administered at the beginning of resuscitation. Mice were sacrificed 6h after induction of HS. Plasma levels of IL-6, IL-1?, IL-10, TNF?, KC, MCP-1, and GM-CSF were determined by ELISA. Myeloperoxidase (MPO) activity in pulmonary and liver tissues was analysed with standardised MPO kits.In mice treated with high-dose GW0742, plasma levels of IL-6, IL-1?, and MCP-1 were significantly increased compared to the control group mice. When compared to mice treated with low-dose GW0742 plasma levels of IL-6, IL-1?, GM-CSF, KC, and MCP-1 were significantly elevated in high-dose-treated mice. Low-dose GW0742 treatment was associated with a non-significant downtrend of inflammatory factors in mice with HS. No significant changes of MPO activity in lung and liver were observed between the control group and the GW0742 treatment groups.This study identified dose-dependent effects of GW0742 on systemic inflammation after HS. While high-dose GW0742 substantially enhanced the systemic inflammatory response, low-dose GW0742 led to a downtrend of pro-inflammation cytokine expression. The exact mechanisms are yet unknown and need to be assessed in further studies.
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PPAR?/? agonists are known to modulate the systemic inflammatory response after sepsis. In this study, inflammation modulation effects of PPAR?/? are investigated using the selective PPAR?/? agonist (GW0742) in a model of haemorrhagic shock (HS)-induced sterile systemic inflammation.Blood pressure-controlled (35±5mmHg) HS was performed in C57/BL6 mice for 90min. Low-dose GW0742 (0.03mg/kg/BW) and high-dose GW0742 (0.3mg/kg/BW) were then administered at the beginning of resuscitation. Mice were s...
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