Myeloid DAP12-associating lectin (MDL)-1 regulates synovial inflammation and bone erosion associated with autoimmune arthritis

DNAX adaptor protein 12 (DAP12) is a trans-membrane adaptor molecule that transduces activating signals in NK and myeloid cells. Absence of functional Dap12 results in osteoclast defects and bone abnormalities. Because DAP12 has no extracelluar binding domains, it must pair with cell surface recepto...

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Autores principales: Joyce-Shaikh, Barbara, Bigler, Michael E., Chao, Cheng-Chi, Murphy, Erin E., Blumenschein, Wendy M., Adamopoulos, Iannis E., Heyworth, Paul G., Antonenko, Svetlana, Bowman, Edward P., McClanahan, Terrill K., Phillips, Joseph H., Cua, Daniel J.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2010
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2839155/
https://www.ncbi.nlm.nih.gov/pubmed/20212065
http://dx.doi.org/10.1084/jem.20090516
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author Joyce-Shaikh, Barbara
Bigler, Michael E.
Chao, Cheng-Chi
Murphy, Erin E.
Blumenschein, Wendy M.
Adamopoulos, Iannis E.
Heyworth, Paul G.
Antonenko, Svetlana
Bowman, Edward P.
McClanahan, Terrill K.
Phillips, Joseph H.
Cua, Daniel J.
author_facet Joyce-Shaikh, Barbara
Bigler, Michael E.
Chao, Cheng-Chi
Murphy, Erin E.
Blumenschein, Wendy M.
Adamopoulos, Iannis E.
Heyworth, Paul G.
Antonenko, Svetlana
Bowman, Edward P.
McClanahan, Terrill K.
Phillips, Joseph H.
Cua, Daniel J.
author_sort Joyce-Shaikh, Barbara
collection PubMed
description DNAX adaptor protein 12 (DAP12) is a trans-membrane adaptor molecule that transduces activating signals in NK and myeloid cells. Absence of functional Dap12 results in osteoclast defects and bone abnormalities. Because DAP12 has no extracelluar binding domains, it must pair with cell surface receptors for signal transduction. There are at least 15 known DAP12-associating cell surface receptors with distinct temporal and cell type–specific expression patterns. Our aim was to determine which receptors may be important in DAP12-associated bone pathologies. Here, we identify myeloid DAP12-associating lectin (MDL)-1 receptor (also known as CLEC5A) as a key regulator of synovial injury and bone erosion during autoimmune joint inflammation. Activation of MDL-1 leads to enhanced recruitment of inflammatory macrophages and neutrophils to the joint and promotes bone erosion. Functional blockade of MDL-1 receptor via Mdl1 deletion or treatment with MDL-1-Ig fusion protein reduces the clinical signs of autoimmune joint inflammation. These findings suggest that MDL-1 receptor may be a therapeutic target for treatment of immune-mediated skeletal disorders.
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spelling pubmed-28391552010-09-15 Myeloid DAP12-associating lectin (MDL)-1 regulates synovial inflammation and bone erosion associated with autoimmune arthritis Joyce-Shaikh, Barbara Bigler, Michael E. Chao, Cheng-Chi Murphy, Erin E. Blumenschein, Wendy M. Adamopoulos, Iannis E. Heyworth, Paul G. Antonenko, Svetlana Bowman, Edward P. McClanahan, Terrill K. Phillips, Joseph H. Cua, Daniel J. J Exp Med Article DNAX adaptor protein 12 (DAP12) is a trans-membrane adaptor molecule that transduces activating signals in NK and myeloid cells. Absence of functional Dap12 results in osteoclast defects and bone abnormalities. Because DAP12 has no extracelluar binding domains, it must pair with cell surface receptors for signal transduction. There are at least 15 known DAP12-associating cell surface receptors with distinct temporal and cell type–specific expression patterns. Our aim was to determine which receptors may be important in DAP12-associated bone pathologies. Here, we identify myeloid DAP12-associating lectin (MDL)-1 receptor (also known as CLEC5A) as a key regulator of synovial injury and bone erosion during autoimmune joint inflammation. Activation of MDL-1 leads to enhanced recruitment of inflammatory macrophages and neutrophils to the joint and promotes bone erosion. Functional blockade of MDL-1 receptor via Mdl1 deletion or treatment with MDL-1-Ig fusion protein reduces the clinical signs of autoimmune joint inflammation. These findings suggest that MDL-1 receptor may be a therapeutic target for treatment of immune-mediated skeletal disorders. The Rockefeller University Press 2010-03-15 /pmc/articles/PMC2839155/ /pubmed/20212065 http://dx.doi.org/10.1084/jem.20090516 Text en © 2010 Joyce-Shaikh et al. This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 3.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/3.0/).
spellingShingle Article
Joyce-Shaikh, Barbara
Bigler, Michael E.
Chao, Cheng-Chi
Murphy, Erin E.
Blumenschein, Wendy M.
Adamopoulos, Iannis E.
Heyworth, Paul G.
Antonenko, Svetlana
Bowman, Edward P.
McClanahan, Terrill K.
Phillips, Joseph H.
Cua, Daniel J.
Myeloid DAP12-associating lectin (MDL)-1 regulates synovial inflammation and bone erosion associated with autoimmune arthritis
title Myeloid DAP12-associating lectin (MDL)-1 regulates synovial inflammation and bone erosion associated with autoimmune arthritis
title_full Myeloid DAP12-associating lectin (MDL)-1 regulates synovial inflammation and bone erosion associated with autoimmune arthritis
title_fullStr Myeloid DAP12-associating lectin (MDL)-1 regulates synovial inflammation and bone erosion associated with autoimmune arthritis
title_full_unstemmed Myeloid DAP12-associating lectin (MDL)-1 regulates synovial inflammation and bone erosion associated with autoimmune arthritis
title_short Myeloid DAP12-associating lectin (MDL)-1 regulates synovial inflammation and bone erosion associated with autoimmune arthritis
title_sort myeloid dap12-associating lectin (mdl)-1 regulates synovial inflammation and bone erosion associated with autoimmune arthritis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2839155/
https://www.ncbi.nlm.nih.gov/pubmed/20212065
http://dx.doi.org/10.1084/jem.20090516
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