Plasmin and plasminogen prevent sepsis severity by reducing neutrophil extracellular traps and systemic inflammation.
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2023
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Sepsis is a lethal syndrome characterized by systemic inflammation and abnormal coagulation.
Despite therapeutic advances, sepsis mortality remains substantially high. Herein, we investigated
the role of the plasminogen/plasmin (Plg/Pla) system during sepsis. Plasma levels of Plg were
significantly lower in mice subjected to severe compared with nonsevere sepsis, whereas systemic
levels of IL-6, a marker of sepsis severity, were higher in severe sepsis. Plg levels correlated
negatively with IL-6 in both septic mice and patients, whereas plasminogen activator inhibitor-1
levels correlated positively with IL-6. Plg deficiency render mice susceptible to nonsevere sepsis
induced by cecal ligation and puncture (CLP), resulting in greater numbers of neutrophils and M1
macrophages, liver fibrin(ogen) deposition, lower efferocytosis, and increased IL-6 and neutrophil
extracellular trap (NET) release associated with organ damage. Conversely, inflammatory features,
fibrin(ogen), and organ damage were substantially reduced, and efferocytosis was increased by
exogenous Pla given during CLP- and LPS-induced endotoxemia. Plg or Pla protected mice from
sepsis-induced lethality and enhanced the protective effect of antibiotics. Mechanistically, Plg/Pla–
afforded protection was associated with regulation of NET release, requiring Pla-protease activity
and lysine binding sites. Plg/Pla are important host-protective players during sepsis, controlling
local and systemic inflammation and collateral organ damage.
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SILVA, J. P. V. da et al. Plasmin and plasminogen prevent sepsis severity by reducing neutrophil extracellular traps and systemic inflammation. JCI Insight, v. 14, artigo e166044, 2023. Disponível em: <https://insight.jci.org/articles/view/166044/pdf>. Acesso em: 01 ago. 2023.