Augmenting MNK1/2 activation by c-FMS proteolysis promotes osteoclastogenesis and arthritic bone erosion.
Se Hwan MunSeyeon BaeSteven ZengBrian OhCarmen ChaiMatthew Jundong KimHaemin KimGeorge KallioliasChitra Lekha DahiaYounseo OhTae Hwan KimJong Dae JiKyung Hyung Park-MinPublished in: Bone research (2021)
Osteoclasts are bone-resorbing cells that play an essential role in homeostatic bone remodeling and pathological bone erosion. Macrophage colony stimulating factor (M-CSF) is abundant in rheumatoid arthritis (RA). However, the role of M-CSF in arthritic bone erosion is not completely understood. Here, we show that M-CSF can promote osteoclastogenesis by triggering the proteolysis of c-FMS, a receptor for M-CSF, leading to the generation of FMS intracellular domain (FICD) fragments. Increased levels of FICD fragments positively regulated osteoclastogenesis but had no effect on inflammatory responses. Moreover, myeloid cell-specific FICD expression in mice resulted in significantly increased osteoclast-mediated bone resorption in an inflammatory arthritis model. The FICD formed a complex with DAP5, and the FICD/DAP5 axis promoted osteoclast differentiation by activating the MNK1/2/EIF4E pathway and enhancing NFATc1 protein expression. Moreover, targeting the MNK1/2 pathway diminished arthritic bone erosion. These results identified a novel role of c-FMS proteolysis in osteoclastogenesis and the pathogenesis of arthritic bone erosion.
Keyphrases
- bone loss
- bone mineral density
- rheumatoid arthritis
- tyrosine kinase
- soft tissue
- bone regeneration
- oxidative stress
- adipose tissue
- poor prognosis
- skeletal muscle
- induced apoptosis
- transcription factor
- single cell
- ankylosing spondylitis
- binding protein
- reactive oxygen species
- immune response
- long non coding rna
- mesenchymal stem cells
- cell proliferation
- insulin resistance
- wild type