Lectins offer new perspectives in the development of macrophage-targeted therapies for COPD/emphysema.

Lectins offer new perspectives in the development of macrophage-targeted therapies for COPD/emphysema.

We have previously shown that the defective ability of alveolar macrophages (AM) to phagocytose apoptotic cells ('efferocytosis') in chronic obstructive pulmonary disease/emphysema (COPD) could be therapeutically improved using the C-type lectin, mannose binding lectin (MBL), although the...

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Main Authors: Violet R Mukaro, Johan Bylund, Greg Hodge, Mark Holmes, Hubertus Jersmann, Paul N Reynolds, Sandra Hodge
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23441163/?tool=EBI
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spelling doaj-58442b7977224fb8ac2766c1c3df03492021-03-03T23:42:48ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0182e5614710.1371/journal.pone.0056147Lectins offer new perspectives in the development of macrophage-targeted therapies for COPD/emphysema.Violet R MukaroJohan BylundGreg HodgeMark HolmesHubertus JersmannPaul N ReynoldsSandra HodgeWe have previously shown that the defective ability of alveolar macrophages (AM) to phagocytose apoptotic cells ('efferocytosis') in chronic obstructive pulmonary disease/emphysema (COPD) could be therapeutically improved using the C-type lectin, mannose binding lectin (MBL), although the exact mechanisms underlying this effect are unknown. An S-type lectin, galectin-3, is also known to regulate macrophage phenotype and function, via interaction with its receptor CD98. We hypothesized that defective expression of galectin/CD98 would be associated with defective efferocytosis in COPD and that mechanisms would include effects on cytoskeletal remodeling and macrophage phenotype and glutathione (GSH) availability. Galectin-3 was measured by ELISA in BAL from controls, smokers and current/ex-smokers with COPD. CD98 was measured on AM using flow cytometry. We assessed the effects of galectin-3 on efferocytosis, CD98, GSH, actin polymerisation, rac activation, and the involvement of PI3K (using β-actin probing and wortmannin inhibition) in vitro using human AM and/or MH-S macrophage cell line. Significant decreases in BAL galectin-3 and AM CD98 were observed in BAL from both current- and ex-smoker COPD subjects vs controls. Galectin 3 increased efferocytosis via an increase in active GTP bound Rac1. This was confirmed with β-actin probing and the role of PI3K was confirmed using wortmannin inhibition. The increased efferocytosis was associated with increases in available glutathione and expression of CD98. We provide evidence for a role of airway lectins in the failed efferocytosis in COPD, supporting their further investigation as potential macrophage-targeted therapies.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23441163/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Violet R Mukaro
Johan Bylund
Greg Hodge
Mark Holmes
Hubertus Jersmann
Paul N Reynolds
Sandra Hodge
spellingShingle Violet R Mukaro
Johan Bylund
Greg Hodge
Mark Holmes
Hubertus Jersmann
Paul N Reynolds
Sandra Hodge
Lectins offer new perspectives in the development of macrophage-targeted therapies for COPD/emphysema.
PLoS ONE
author_facet Violet R Mukaro
Johan Bylund
Greg Hodge
Mark Holmes
Hubertus Jersmann
Paul N Reynolds
Sandra Hodge
author_sort Violet R Mukaro
title Lectins offer new perspectives in the development of macrophage-targeted therapies for COPD/emphysema.
title_short Lectins offer new perspectives in the development of macrophage-targeted therapies for COPD/emphysema.
title_full Lectins offer new perspectives in the development of macrophage-targeted therapies for COPD/emphysema.
title_fullStr Lectins offer new perspectives in the development of macrophage-targeted therapies for COPD/emphysema.
title_full_unstemmed Lectins offer new perspectives in the development of macrophage-targeted therapies for COPD/emphysema.
title_sort lectins offer new perspectives in the development of macrophage-targeted therapies for copd/emphysema.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description We have previously shown that the defective ability of alveolar macrophages (AM) to phagocytose apoptotic cells ('efferocytosis') in chronic obstructive pulmonary disease/emphysema (COPD) could be therapeutically improved using the C-type lectin, mannose binding lectin (MBL), although the exact mechanisms underlying this effect are unknown. An S-type lectin, galectin-3, is also known to regulate macrophage phenotype and function, via interaction with its receptor CD98. We hypothesized that defective expression of galectin/CD98 would be associated with defective efferocytosis in COPD and that mechanisms would include effects on cytoskeletal remodeling and macrophage phenotype and glutathione (GSH) availability. Galectin-3 was measured by ELISA in BAL from controls, smokers and current/ex-smokers with COPD. CD98 was measured on AM using flow cytometry. We assessed the effects of galectin-3 on efferocytosis, CD98, GSH, actin polymerisation, rac activation, and the involvement of PI3K (using β-actin probing and wortmannin inhibition) in vitro using human AM and/or MH-S macrophage cell line. Significant decreases in BAL galectin-3 and AM CD98 were observed in BAL from both current- and ex-smoker COPD subjects vs controls. Galectin 3 increased efferocytosis via an increase in active GTP bound Rac1. This was confirmed with β-actin probing and the role of PI3K was confirmed using wortmannin inhibition. The increased efferocytosis was associated with increases in available glutathione and expression of CD98. We provide evidence for a role of airway lectins in the failed efferocytosis in COPD, supporting their further investigation as potential macrophage-targeted therapies.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23441163/?tool=EBI
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