5 research outputs found
Characterization and modulation of microglial phenotypes in an animal model of severe sepsis
Get PDFWe aim to characterize the kinetics of early and late microglial phenotypes after systemic inflammation in an animal model of severe sepsis and the effects of minocycline on these phenotypes. Rats were subjected to CLP, and some animals were treated with minocycline (10 ug/kg) by i.c.v. administration. Animals were killed 24 hours, 5, 10 and 30 days after sepsis induction, and serum and hippocampus were collected for subsequent analyses. Realâtime PCR was performed for M1 and M2 markers. TNFâα, ILâ1ÎČ, ILâ6, ILâ10, CCLâ22 and nitrite/nitrate levels were measured. Immunofluorescence for IBAâ1, CD11b and arginase was also performed. We demonstrated that early after sepsis, there was a preponderant upâregulation of M1 markers, and this was not switched to M2 phenotype markers later on. We found that upâregulation of both M1 and M2 markers coâexisted up to 30 days after sepsis induction. In addition, minocycline induced a downâregulation, predominantly, of M1 markers. Our results suggest early activation of M1 microglia that is followed by an overlap of both M1 and M2 phenotypes and that the beneficial effects of minocycline on sepsisâassociated brain dysfunction may be related to its effects predominantly on the M1 phenotype
