| Literature DB >> 30124596 |
Marlies Ballegeer1,2, Jolien Vandewalle1,2, Melanie Eggermont1,2, Gert Van Isterdael1,2, Lien Dejager1,2, Liesbet De Bus3, Johan Decruyenaere3, Roosmarijn E Vandenbroucke1,2, Claude Libert1,2.
Abstract
Sepsis in humans and experimental animals is characterized by an acute inflammatory response. glucocorticoids (GCs) are widely used for the treatment of many inflammatory disorders, yet their effectiveness in sepsis is debatable. One of the major anti-inflammatory proteins induced by GCs is glucocorticoid-induced leucine zipper (GILZ, coded by the TSC22D3 gene). We found that TSC22D3 mRNA expression is downregulated in white blood cells of human sepsis patients. Interestingly, transgenic GILZ-overexpressing mice (GILZ-tg) showed better survival rates in the cecal ligation and puncture (CLP) model of mouse sepsis. To our surprise, GILZ had only mild anti-inflammatory effects in this model, as the systemic proinflammatory response was not significantly reduced in GILZ-tg mice compared with control mice. During CLP, we observed reduced bacterial counts in blood of GILZ-tg mice compared with control mice. We found increased expression of Tsc22d3 mRNA specifically in peritoneal exudate cells in the CLP model, as well as increased capacity for bacterial phagocytosis of CD45 GILZ-tg cells compared with CD45 GILZ-wt cells. Hence, we believe that the protective effects of GILZ in the CLP model can be linked to a more efficient phagocytosis.Entities:
Year: 2019 PMID: 30124596 DOI: 10.1097/SHK.0000000000001252
Source DB: PubMed Journal: Shock ISSN: 1073-2322 Impact factor: 3.454