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Role of plasma kallikrein–kinin system activation in synovial recruitment of endothelial progenitor cells in experimental arthritis
Author(s) -
Dai Jihong,
Agelan Alexis,
Yang Aizhen,
Zuluaga Viviana,
Sexton Daniel,
Colman Robert W.,
Wu Yi
Publication year - 2012
Publication title -
arthritis & rheumatism
Language(s) - English
Resource type - Journals
eISSN - 1529-0131
pISSN - 0004-3591
DOI - 10.1002/art.34607
Subject(s) - progenitor cell , bradykinin , kinin , kallikrein , arthritis , synovitis , endocrinology , immunology , medicine , cancer research , receptor , chemistry , microbiology and biotechnology , biology , stem cell , biochemistry , enzyme
Objective To examine whether activation of the plasma kallikrein–kinin system (KKS) mediates synovial recruitment of endothelial progenitor cells (EPCs) in arthritis. Methods EPCs were isolated from Lewis rat bone marrow, and expression of progenitor cell–lineage markers and functional properties were characterized. EPCs were injected intravenously into Lewis rats with arthritis, and their recruitment and formation of de novo blood vessels in inflamed synovium were evaluated. The role of plasma KKS was examined using a plasma kallikrein inhibitor (EPI‐KAL2) and an antikallikrein antibody (13G11). A transendothelial migration assay was used to determine the role of bradykinin and its receptor in EPC mobilization. Results EPCs from Lewis rats exhibited a strong capacity to form tubes and vacuoles and expressed increased levels of bradykinin type 2 receptor (B2R) and progenitor cell markers CD34 and Sca‐1. In Lewis rats with arthritis, EPCs were recruited into inflamed synovium at the acute phase of disease and formed de novo blood vessels. Inhibition of plasma kallikrein by EPI‐KAL2 and 13G11 significantly suppressed synovial recruitment of EPCs and hyperproliferation of synovial cells. Bradykinin stimulated transendothelial migration of EPCs in a concentration‐dependent manner. This was mediated by B2R, as demonstrated by the finding that knockdown of B2R with silencing RNA completely blocked bradykinin‐stimulated transendothelial migration. Moreover, bradykinin selectively up‐regulated expression of the homing receptor CXCR4 in EPCs. Conclusion These observations demonstrate a novel role of plasma KKS activation in the synovial recruitment of EPCs in arthritis, acting via kallikrein activation and B2R‐dependent mechanisms. B2R might be involved in the mobilization of EPCs via up‐regulation of CXCR4.

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