| Literature DB >> 30509116 |
Tae-Hyung Kim1,2, Chau Ly1,3, Alexei Christodoulides1, Cameron J Nowell4, Peter W Gunning5, Erica K Sloan2,6,4,7,8, Amy C Rowat1,3,6.
Abstract
Critical functions of immune cells require them to rapidly change their shape and generate forces in response to cues from their surrounding environment. However, little is known about how soluble factors that may be present in the microenvironment modulate key aspects of cellular mechanobiology-such as immune cell deformability and force generation-to impact functions such as phagocytosis and migration. Here we show that signaling by soluble stress hormones through β-adrenoceptors (β-AR) reduces the deformability of macrophages; this is dependent on changes in the organization of the actin cytoskeleton and is associated with functional changes in phagocytosis and migration. Pharmacologic interventions reveal that the impact of β-AR signaling on macrophage deformability is dependent on actin-related proteins 2/3, indicating that stress hormone signaling through β-AR shifts actin organization to favor branched structures rather than linear unbranched actin filaments. These findings show that through remodeling of the actin cytoskeleton, β-AR-mediated stress hormone signaling modulates macrophage mechanotype to impact functions that play a critical role in immune response.-Kim, T.-H., Ly, C., Christodoulides, A., Nowell, C. J., Gunning, P. W., Sloan, E. K., Rowat, A. C. Stress hormone signaling through β-adrenergic receptors regulates macrophage mechanotype and function.Entities:
Keywords: actin; chemotaxis; deformability; phagocytosis
Mesh:
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Year: 2018 PMID: 30509116 PMCID: PMC6404566 DOI: 10.1096/fj.201801429RR
Source DB: PubMed Journal: FASEB J ISSN: 0892-6638 Impact factor: 5.834