High-Affinity Bent β(2)-Integrin Molecules in Arresting Neutrophils Face Each Other through Binding to ICAMs In cis

Leukocyte adhesion requires β(2)-integrin activation. Resting integrins exist in a bent-closed conformation—i.e., not extended (E(−)) and not high affinity (H(−))—unable to bind ligand. Fully activated E(+)H(+) integrin binds intercellular adhesion molecules (ICAMs) expressed on the opposing cell in...

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Autores principales: Fan, Zhichao, Kiosses, William Bill, Sun, Hao, Orecchioni, Marco, Ghosheh, Yanal, Zajonc, Dirk M., Arnaout, M. Amin, Gutierrez, Edgar, Groisman, Alex, Ginsberg, Mark H., Ley, Klaus
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2019
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6625519/
https://www.ncbi.nlm.nih.gov/pubmed/30605669
http://dx.doi.org/10.1016/j.celrep.2018.12.038
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author Fan, Zhichao
Kiosses, William Bill
Sun, Hao
Orecchioni, Marco
Ghosheh, Yanal
Zajonc, Dirk M.
Arnaout, M. Amin
Gutierrez, Edgar
Groisman, Alex
Ginsberg, Mark H.
Ley, Klaus
author_facet Fan, Zhichao
Kiosses, William Bill
Sun, Hao
Orecchioni, Marco
Ghosheh, Yanal
Zajonc, Dirk M.
Arnaout, M. Amin
Gutierrez, Edgar
Groisman, Alex
Ginsberg, Mark H.
Ley, Klaus
author_sort Fan, Zhichao
collection PubMed
description Leukocyte adhesion requires β(2)-integrin activation. Resting integrins exist in a bent-closed conformation—i.e., not extended (E(−)) and not high affinity (H(−))—unable to bind ligand. Fully activated E(+)H(+) integrin binds intercellular adhesion molecules (ICAMs) expressed on the opposing cell in trans. E(−)H(−) transitions to E(+)H(+) through E(+)H(−) or through EH(+), which binds to ICAMs on the same cell in cis. Spatial patterning of activated integrins is thought to be required for effective arrest, but no high-resolution cell surface localization maps of activated integrins exist. Here, we developed Super-STORM by combining super-resolution microscopy with molecular modeling to precisely localize activated integrin molecules and identify the molecular patterns of activated integrins on primary human neutrophils. At the time of neutrophil arrest, E(−)H(+) integrins face each other to form oriented (non-random) nanoclusters. To address the mechanism causing this pattern, we blocked integrin binding to ICAMs in cis, which significantly relieved the face-to-face orientation.
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spelling pubmed-66255192019-07-12 High-Affinity Bent β(2)-Integrin Molecules in Arresting Neutrophils Face Each Other through Binding to ICAMs In cis Fan, Zhichao Kiosses, William Bill Sun, Hao Orecchioni, Marco Ghosheh, Yanal Zajonc, Dirk M. Arnaout, M. Amin Gutierrez, Edgar Groisman, Alex Ginsberg, Mark H. Ley, Klaus Cell Rep Article Leukocyte adhesion requires β(2)-integrin activation. Resting integrins exist in a bent-closed conformation—i.e., not extended (E(−)) and not high affinity (H(−))—unable to bind ligand. Fully activated E(+)H(+) integrin binds intercellular adhesion molecules (ICAMs) expressed on the opposing cell in trans. E(−)H(−) transitions to E(+)H(+) through E(+)H(−) or through EH(+), which binds to ICAMs on the same cell in cis. Spatial patterning of activated integrins is thought to be required for effective arrest, but no high-resolution cell surface localization maps of activated integrins exist. Here, we developed Super-STORM by combining super-resolution microscopy with molecular modeling to precisely localize activated integrin molecules and identify the molecular patterns of activated integrins on primary human neutrophils. At the time of neutrophil arrest, E(−)H(+) integrins face each other to form oriented (non-random) nanoclusters. To address the mechanism causing this pattern, we blocked integrin binding to ICAMs in cis, which significantly relieved the face-to-face orientation. 2019-01-02 /pmc/articles/PMC6625519/ /pubmed/30605669 http://dx.doi.org/10.1016/j.celrep.2018.12.038 Text en This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Fan, Zhichao
Kiosses, William Bill
Sun, Hao
Orecchioni, Marco
Ghosheh, Yanal
Zajonc, Dirk M.
Arnaout, M. Amin
Gutierrez, Edgar
Groisman, Alex
Ginsberg, Mark H.
Ley, Klaus
High-Affinity Bent β(2)-Integrin Molecules in Arresting Neutrophils Face Each Other through Binding to ICAMs In cis
title High-Affinity Bent β(2)-Integrin Molecules in Arresting Neutrophils Face Each Other through Binding to ICAMs In cis
title_full High-Affinity Bent β(2)-Integrin Molecules in Arresting Neutrophils Face Each Other through Binding to ICAMs In cis
title_fullStr High-Affinity Bent β(2)-Integrin Molecules in Arresting Neutrophils Face Each Other through Binding to ICAMs In cis
title_full_unstemmed High-Affinity Bent β(2)-Integrin Molecules in Arresting Neutrophils Face Each Other through Binding to ICAMs In cis
title_short High-Affinity Bent β(2)-Integrin Molecules in Arresting Neutrophils Face Each Other through Binding to ICAMs In cis
title_sort high-affinity bent β(2)-integrin molecules in arresting neutrophils face each other through binding to icams in cis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6625519/
https://www.ncbi.nlm.nih.gov/pubmed/30605669
http://dx.doi.org/10.1016/j.celrep.2018.12.038
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