1. Cytohesin-2/ARNO: A Novel Bridge Between Cell Migration and Immunoregulation in Synovial Fibroblasts
- Author
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Yilin Wang, Çağlar Çil, Margaret M. Harnett, and Miguel A. Pineda
- Subjects
musculoskeletal diseases ,STAT3 Transcription Factor ,Interleukin-1beta ,Immunology ,Gene Expression ,ARNO ,Immunomodulation ,Mice ,arthritis (including rheumatoid arthritis) ,Cell Movement ,Animals ,Immunology and Allergy ,Phosphorylation ,RNA, Small Interfering ,Original Research ,GTPase-Activating Proteins ,Synovial Membrane ,RC581-607 ,Fibroblasts ,synovial fibroblast (FLS) ,ADP-Ribosylation Factor 6 ,inflammation ,Cytokines ,cytohesin 2 ,Immunologic diseases. Allergy ,Biomarkers ,Signal Transduction - Abstract
The guanine nucleotide exchange factor cytohesin-2 (ARNO) is a major activator of the small GTPase ARF6 that has been shown to play an important role(s) in cell adhesion, migration and cytoskeleton reorganization in various cell types and models of disease. Interestingly, dysregulated cell migration, in tandem with hyper-inflammatory responses, is one of the hallmarks associated with activated synovial fibroblasts (SFs) during chronic inflammatory joint diseases, like rheumatoid arthritis. The role of ARNO in this process has previously been unexplored but we hypothesized that the pro-inflammatory milieu of inflamed joints locally induces activation of ARNO-mediated pathways in SFs, promoting an invasive cell phenotype that ultimately leads to bone and cartilage damage. Thus, we used small interference RNA to investigate the impact of ARNO on the pathological migration and inflammatory responses of murine SFs, revealing a fully functional ARNO-ARF6 pathway which can be rapidly activated by IL-1β. Such signalling promotes cell migration and formation of focal adhesions. Unexpectedly, ARNO was also shown to modulate SF-inflammatory responses, dictating their precise cytokine and chemokine expression profile. Our results uncover a novel role for ARNO in SF-dependent inflammation, that potentially links pathogenic migration with initiation of local joint inflammation, offering new approaches for targeting the fibroblast compartment in chronic arthritis and joint disease.
- Published
- 2022
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