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Differential attenuation of ?2 integrin-dependent and -independent neutrophil migration by Ly6G ligation.


ABSTRACT: Antibody ligation of the murine neutrophil surface protein Ly6G disrupts neutrophil migration in some contexts but not others. We tested whether this variability reflected divergent dependence of neutrophil migration on ?2 integrins, adhesion molecules that interact with Ly6G at the neutrophil surface. In integrin-dependent murine arthritis, Ly6G ligation attenuated joint inflammation, even though mice lacking Ly6G altogether developed arthritis normally. By contrast, Ly6G ligation had no impact on integrin-independent neutrophil migration into inflamed lung. In peritoneum, the role of ?2 integrins varied with stimulus, proving dispensable for neutrophil entry in Escherichia coli peritonitis but contributory in interleukin 1 (IL-1)-mediated sterile peritonitis. Correspondingly, Ly6G ligation attenuated only IL-1 peritonitis, disrupting the molecular association between integrins and Ly6G and inducing cell-intrinsic blockade restricted to integrin-dependent migration. Consistent with this observation, Ly6G ligation impaired integrin-mediated postadhesion strengthening for neutrophils arresting on activated cremaster endothelium in vivo. Together, these findings identify selective inhibition of integrin-mediated neutrophil emigration through Ly6G ligation, highlighting the marked site and stimulus specificity of ?2 integrin dependence in neutrophil migration.

SUBMITTER: Cunin P 

PROVIDER: S-EPMC6373735 | biostudies-literature | 2019 Feb

REPOSITORIES: biostudies-literature

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Differential attenuation of β2 integrin-dependent and -independent neutrophil migration by Ly6G ligation.

Cunin Pierre P   Lee Pui Y PY   Kim Edy E   Schmider Angela B AB   Cloutier Nathalie N   Pare Alexandre A   Gunzer Matthias M   Soberman Roy J RJ   Lacroix Steve S   Boilard Eric E   Lefort Craig T CT   Nigrovic Peter A PA  

Blood advances 20190201 3


Antibody ligation of the murine neutrophil surface protein Ly6G disrupts neutrophil migration in some contexts but not others. We tested whether this variability reflected divergent dependence of neutrophil migration on β2 integrins, adhesion molecules that interact with Ly6G at the neutrophil surface. In integrin-dependent murine arthritis, Ly6G ligation attenuated joint inflammation, even though mice lacking Ly6G altogether developed arthritis normally. By contrast, Ly6G ligation had no impact  ...[more]

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