Bcl3 prevents acute inflammatory lung injury in mice by restraining emergency granulopoiesis
Daniel Kreisel, … , Ruaidhri J. Carmody, Andrew E. Gelman
Daniel Kreisel, … , Ruaidhri J. Carmody, Andrew E. Gelman
Published December 13, 2010
Citation Information: J Clin Invest. 2011;121(1):265-276. https://doi.org/10.1172/JCI42596.
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Research Article Inflammation

Bcl3 prevents acute inflammatory lung injury in mice by restraining emergency granulopoiesis

Abstract

Granulocytes are pivotal regulators of tissue injury. However, the transcriptional mechanisms that regulate granulopoiesis under inflammatory conditions are poorly understood. Here we show that the transcriptional coregulator B cell leukemia/lymphoma 3 (Bcl3) limits granulopoiesis under emergency (i.e., inflammatory) conditions, but not homeostatic conditions. Treatment of mouse myeloid progenitors with G-CSF — serum concentrations of which rise under inflammatory conditions — rapidly increased Bcl3 transcript accumulation in a STAT3-dependent manner. Bcl3-deficient myeloid progenitors demonstrated an enhanced capacity to proliferate and differentiate into granulocytes following G-CSF stimulation, whereas the accumulation of Bcl3 protein attenuated granulopoiesis in an NF-κB p50–dependent manner. In a clinically relevant model of transplant-mediated lung ischemia reperfusion injury, expression of Bcl3 in recipients inhibited emergency granulopoiesis and limited acute graft damage. These data demonstrate a critical role for Bcl3 in regulating emergency granulopoiesis and suggest that targeting the differentiation of myeloid progenitors may be a therapeutic strategy for preventing inflammatory lung injury.

Authors

Daniel Kreisel, Seiichiro Sugimoto, Jeremy Tietjens, Jihong Zhu, Sumiharu Yamamoto, Alexander S. Krupnick, Ruaidhri J. Carmody, Andrew E. Gelman

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Figure 6

G-CSF blockade prevents graft injury in B6 (Bcl3–/–) lung recipients.

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G-CSF blockade prevents graft injury in B6 (Bcl3–/–) lung recipients. ...
(A) Granulocyte numbers in the peripheral blood (left) and BAL (middle) at 6 and 24 hours post-engraftment and a representative FACS analysis (24 hours; right) in which numbers indicate granulocyte percent abundance in graft tissue in B6 → B6 (Bcl3–/–) lung recipients treated with control Ig or G-CSF–specific antibodies (n = 10). (B) PaO2 (left) and EBD exclusion (middle) 6 and 24 hours post-engraftment and representative graft histology (right; original magnification, ×100) in B6 → B6 (Bcl3–/–) lung graft recipients 24 hours after engraftment treated with control Ig or G-CSF–specific antibodies (n = 10). Data represent mean ± SD. *P < 0.05.