Publication | Open Access
Origin of Circulating Free DNA in Sepsis: Analysis of the CLP Mouse Model
54
Citations
25
References
2015
Year
Histone H3Laboratory ImmunologyImmunologyPathologyCirculating Free DnaImmune SystemFree DnaInflammationCitrullinated Histone H3ImmunopathologyMolecular DiagnosticsClp Mouse ModelKnockout MouseAutoimmune DiseaseGranulocyteDna ReplicationAutoimmunityImmune Cell DevelopmentPathogenesisMedicineImmunological Biomarkers
Recently, it has been reported that circulating free DNA (cf-DNA) in the blood is increased in various infectious diseases, including sepsis. Moreover, a relationship between cf-DNA and neutrophil extracellular traps (NETs) has been suggested. However, it is still unclear what the source and physiological role of cf-DNA in sepsis are. In this study, we examined the source of cf-DNA by detecting citrullinated histone H3, a characteristic feature of NET formation, in cecal ligation and puncture- (CLP-)operated mice. In addition, neutrophil depletion using anti-Ly6G antibodies was performed to assess the association between neutrophils and cf-DNA. Increased cf-DNA levels were observed only in CLP mice and not in the control groups; the qPCR findings revealed that the cf-DNA was mainly host-derived, even in bacteremic conditions. Citrullinated histone H3 was not increased in the neutrophils upon CLP, and the depletion of neutrophils showed limited effects on decreasing the amount of cf-DNA. Taken together, these results suggested that elevated cf-DNA levels during early-phase sepsis may represent a candidate biomarker for the severity of sepsis and that, contrary to previous findings, cf-DNA is not derived from neutrophils or NETs.
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