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Publication : Frontline Science: The expression of integrin α<sub>D</sub> β<sub>2</sub> (CD11d/CD18) on neutrophils orchestrates the defense mechanism against endotoxemia and sepsis.

First Author  Bailey WP Year  2021
Journal  J Leukoc Biol Volume  109
Issue  5 Pages  877-890
PubMed ID  33438263 Mgi Jnum  J:305404
Mgi Id  MGI:6696282 Doi  10.1002/JLB.3HI0820-529RR
Citation  Bailey WP, et al. (2021) Frontline Science: The expression of integrin alphaD beta2 (CD11d/CD18) on neutrophils orchestrates the defense mechanism against endotoxemia and sepsis. J Leukoc Biol 109(5):877-890
abstractText  Neutrophil-macrophage interplay is a fine-tuning mechanism that regulates the innate immune response during infection and inflammation. Cell surface receptors play an essential role in neutrophil and macrophage functions. The same receptor can provide different outcomes within diverse leukocyte subsets in different inflammatory conditions. Understanding the variety of responses mediated by one receptor is critical for the development of anti-inflammatory treatments. In this study, we evaluated the role of a leukocyte adhesive receptor, integrin alphaD beta2 , in the development of acute inflammation. alphaD beta2 is mostly expressed on macrophages and contributes to the development of chronic inflammation. In contrast, we found that alphaD -knockout dramatically increases mortality in the cecal ligation and puncture sepsis model and LPS-induced endotoxemia. This pathologic outcome of alphaD -deficient mice is associated with a reduced number of monocyte-derived macrophages and an increased number of neutrophils in their lungs. However, the tracking of adoptively transferred fluorescently labeled wild-type (WT) and alphaD (-/-) monocytes in WT mice during endotoxemia demonstrated only a moderate difference between the recruitment of these two subsets. Moreover, the rescue experiment, using i.v. injection of WT monocytes to alphaD -deficient mice followed by LPS challenge, showed only slightly reduced mortality. Surprisingly, the injection of WT neutrophils to the bloodstream of alphaD (-/-) mice markedly increased migration of monocyte-derived macrophage to lungs and dramatically improves survival. alphaD -deficient neutrophils demonstrate increased necrosis/pyroptosis. alphaD beta2 -mediated macrophage accumulation in the lungs promotes efferocytosis that reduced mortality. Hence, integrin alphaD beta2 implements a complex defense mechanism during endotoxemia, which is mediated by macrophages via a neutrophil-dependent pathway.
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