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Monocyte Subsets Have Distinct Patterns of Tetraspanin Expression and Different Capacities to Form Multinucleate Giant Cells

Monocytes are able to undergo homotypic fusion to produce different types of multinucleated giant cells, such as Langhans giant cells in response to M. tuberculosis infection or foreign body giant cells in response to implanted biomaterials. Monocyte fusion is highly coordinated and complex, with va...

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Autores principales: Champion, Thomas C., Partridge, Lynda J., Ong, Siew-Min, Malleret, Benoit, Wong, Siew-Cheng, Monk, Peter N.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6002745/
https://www.ncbi.nlm.nih.gov/pubmed/29937768
http://dx.doi.org/10.3389/fimmu.2018.01247
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author Champion, Thomas C.
Partridge, Lynda J.
Ong, Siew-Min
Malleret, Benoit
Wong, Siew-Cheng
Monk, Peter N.
author_facet Champion, Thomas C.
Partridge, Lynda J.
Ong, Siew-Min
Malleret, Benoit
Wong, Siew-Cheng
Monk, Peter N.
author_sort Champion, Thomas C.
collection PubMed
description Monocytes are able to undergo homotypic fusion to produce different types of multinucleated giant cells, such as Langhans giant cells in response to M. tuberculosis infection or foreign body giant cells in response to implanted biomaterials. Monocyte fusion is highly coordinated and complex, with various soluble, intracellular, and cell-surface components mediating different stages of the process. Tetraspanins, such as CD9, CD63, and CD81, are known to be involved in cell:cell fusion and have been suggested to play a role in regulating homotypic monocyte fusion. However, peripheral human monocytes are not homogenous: they exist as a heterogeneous population consisting of three subsets, classical (CD14(++)CD16(−)), intermediate (CD14(++)CD16(+)), and non-classical (CD14(+)CD16(+)), at steady state. During infection with mycobacteria, the circulating populations of intermediate and non-classical monocytes increase, suggesting they may play a role in the disease outcome. Human monocytes were separated into subsets and then induced to fuse using concanavalin A. The intermediate monocytes were able to fuse faster and form significantly larger giant cells than the other subsets. When antibodies targeting tetraspanins were added, the intermediate monocytes responded to anti-CD63 by forming smaller giant cells, suggesting an involvement of tetraspanins in fusion for at least this subset. However, the expression of fusion-associated tetraspanins on monocyte subsets did not correlate with the extent of fusion or with the inhibition by tetraspanin antibody. We also identified a CD9(High) and a CD9(Low) monocyte population within the classical subset. The CD9(High) classical monocytes expressed higher levels of tetraspanin CD151 compared to CD9(Low) classical monocytes but the CD9(High) classical subset did not exhibit greater potential to fuse and the role of these cells in immunity remains unknown. With the exception of dendrocyte-expressed seven transmembrane protein, which was expressed at higher levels on the intermediate monocyte subset, the expression of fusion-related proteins between the subsets did not clearly correlate with their ability to fuse. We also did not observe any clear correlation between giant cell formation and the expression of pro-inflammatory or fusogenic cytokines. Although tetraspanin expression appears to be important for the fusion of intermediate monocytes, the control of multinucleate giant cell formation remains obscure.
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spelling pubmed-60027452018-06-22 Monocyte Subsets Have Distinct Patterns of Tetraspanin Expression and Different Capacities to Form Multinucleate Giant Cells Champion, Thomas C. Partridge, Lynda J. Ong, Siew-Min Malleret, Benoit Wong, Siew-Cheng Monk, Peter N. Front Immunol Immunology Monocytes are able to undergo homotypic fusion to produce different types of multinucleated giant cells, such as Langhans giant cells in response to M. tuberculosis infection or foreign body giant cells in response to implanted biomaterials. Monocyte fusion is highly coordinated and complex, with various soluble, intracellular, and cell-surface components mediating different stages of the process. Tetraspanins, such as CD9, CD63, and CD81, are known to be involved in cell:cell fusion and have been suggested to play a role in regulating homotypic monocyte fusion. However, peripheral human monocytes are not homogenous: they exist as a heterogeneous population consisting of three subsets, classical (CD14(++)CD16(−)), intermediate (CD14(++)CD16(+)), and non-classical (CD14(+)CD16(+)), at steady state. During infection with mycobacteria, the circulating populations of intermediate and non-classical monocytes increase, suggesting they may play a role in the disease outcome. Human monocytes were separated into subsets and then induced to fuse using concanavalin A. The intermediate monocytes were able to fuse faster and form significantly larger giant cells than the other subsets. When antibodies targeting tetraspanins were added, the intermediate monocytes responded to anti-CD63 by forming smaller giant cells, suggesting an involvement of tetraspanins in fusion for at least this subset. However, the expression of fusion-associated tetraspanins on monocyte subsets did not correlate with the extent of fusion or with the inhibition by tetraspanin antibody. We also identified a CD9(High) and a CD9(Low) monocyte population within the classical subset. The CD9(High) classical monocytes expressed higher levels of tetraspanin CD151 compared to CD9(Low) classical monocytes but the CD9(High) classical subset did not exhibit greater potential to fuse and the role of these cells in immunity remains unknown. With the exception of dendrocyte-expressed seven transmembrane protein, which was expressed at higher levels on the intermediate monocyte subset, the expression of fusion-related proteins between the subsets did not clearly correlate with their ability to fuse. We also did not observe any clear correlation between giant cell formation and the expression of pro-inflammatory or fusogenic cytokines. Although tetraspanin expression appears to be important for the fusion of intermediate monocytes, the control of multinucleate giant cell formation remains obscure. Frontiers Media S.A. 2018-06-08 /pmc/articles/PMC6002745/ /pubmed/29937768 http://dx.doi.org/10.3389/fimmu.2018.01247 Text en Copyright © 2018 Champion, Partridge, Ong, Malleret, Wong and Monk. https://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Champion, Thomas C.
Partridge, Lynda J.
Ong, Siew-Min
Malleret, Benoit
Wong, Siew-Cheng
Monk, Peter N.
Monocyte Subsets Have Distinct Patterns of Tetraspanin Expression and Different Capacities to Form Multinucleate Giant Cells
title Monocyte Subsets Have Distinct Patterns of Tetraspanin Expression and Different Capacities to Form Multinucleate Giant Cells
title_full Monocyte Subsets Have Distinct Patterns of Tetraspanin Expression and Different Capacities to Form Multinucleate Giant Cells
title_fullStr Monocyte Subsets Have Distinct Patterns of Tetraspanin Expression and Different Capacities to Form Multinucleate Giant Cells
title_full_unstemmed Monocyte Subsets Have Distinct Patterns of Tetraspanin Expression and Different Capacities to Form Multinucleate Giant Cells
title_short Monocyte Subsets Have Distinct Patterns of Tetraspanin Expression and Different Capacities to Form Multinucleate Giant Cells
title_sort monocyte subsets have distinct patterns of tetraspanin expression and different capacities to form multinucleate giant cells
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6002745/
https://www.ncbi.nlm.nih.gov/pubmed/29937768
http://dx.doi.org/10.3389/fimmu.2018.01247
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