Frontline Science: Myeloid Cell-Specific Deletion of CEBPB Decreases Sepsis-Induced Immunosuppression in Mice
Document Type
Article
Publication Date
8-1-2017
Description
Sepsis inflammation accelerates myeloid cell generation to compensate for rapid mobilization of the myeloid progenitors from bone marrow. This inflammation-driven myelopoiesis, however, generates myeloid progenitors with immunosuppressive functions that are unable to differentiate into mature, innate immune cells. The myeloid-derived suppressor cells (MDSCs) expand markedly in the later phases of sepsis, suppress both innate and adaptive immunity, and thus, elevate mortality. Using a murine model with myeloid-restricted deletion of the C/EBPβ transcription factor, we show that sepsis-induced generation of MDSCs depends on C/EBPβ. C/EBPβ myeloid cell–deficient mice did not generate MDSCs or develop immunosuppression and survived sepsis. However, septic mice still generated Gr1+ CD11b+ myeloid progenitors at the steady-state levels similar to the control sham mice, suggesting that C/EBPβ is not involved in healthy, steady-state myelopoiesis. C/EBPβ-deficient Gr1+ CD11b+ cells generated fewer monocyte- and granulocyte-like colonies than control mice did, indicating reduced proliferation potential, but differentiated normally in response to growth factors. Adoptive transfer of C/EBPβ-deficient Gr1+ CD11b+ cells from late septic mice exacerbated inflammation in control mice undergoing early sepsis, confirming they were not immunosuppressive. These results show that C/EBPβ directs a switch from proinflammatory to repressor myeloid cells and identifies a novel treatment target.
Citation Information
McPeak, Melissa B.; Youssef, Dima; Williams, Danielle A.; Pritchett, Christopher L.; Yao, Zhi Q.; McCall, Charles E.; and El Gazzar, Mohamed. 2017. Frontline Science: Myeloid Cell-Specific Deletion of CEBPB Decreases Sepsis-Induced Immunosuppression in Mice. Journal of Leukocyte Biology. Vol.102(2). 191-200. https://doi.org/10.1189/jlb.4HI1216-537R PMID: 28476751 ISSN: 0741-5400