Circulating exosomes express α4β7 integrin and compete with CD4+ T cells for the binding to Vedolizumab.

Circulating exosomes express α4β7 integrin and compete with CD4+ T cells for the binding to Vedolizumab.

Vedolizumab (VDZ) is a therapeutic monoclonal antibody approved for the treatment of inflammatory bowel diseases (IBD). VDZ selectively binds to the α4β7 integrin and blocks trafficking of a specific subset of gastrointestinal-homing T-lymphocytes to inflamed tissue. Although VDZ has shown promising...

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Main Authors: Rossana Domenis, Marco Marino, Adriana Cifù, Giulia Scardino, Francesco Curcio, Martina Fabris
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2020-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0242342
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spelling doaj-2208c99183fc4736b4edc78834be34172021-03-04T12:28:36ZengPublic Library of Science (PLoS)PLoS ONE1932-62032020-01-011511e024234210.1371/journal.pone.0242342Circulating exosomes express α4β7 integrin and compete with CD4+ T cells for the binding to Vedolizumab.Rossana DomenisMarco MarinoAdriana CifùGiulia ScardinoFrancesco CurcioMartina FabrisVedolizumab (VDZ) is a therapeutic monoclonal antibody approved for the treatment of inflammatory bowel diseases (IBD). VDZ selectively binds to the α4β7 integrin and blocks trafficking of a specific subset of gastrointestinal-homing T-lymphocytes to inflamed tissue. Although VDZ has shown promising results in numerous clinical studies a subgroup of patients do not respond adequately. Mechanistic insights and prognostic biomarkers able to predict which patients might benefit from VDZ therapy are currently lacking. Circulating exosomes were isolated from serum of blood donors and VDZ-treated patients by polymer-based precipitation. The surface expression of α4β7 integrin was evaluated by flow cytometry and the levels of exosome-bound VDZ were investigated by Promonitor-VDZ ELISA kit. The capacity of exosomes to interfere with the adhesion of VDZ-treated CD4+ T cells was assessed by adhesion assay. In this study, we showed that serum exosomes isolated from both blood donor and ulcerative colitis patients express on their surface the VDZ target α4β7 integrin. We observed an increased exosomal sequestration of VDZ in anti-TNF exposed patients compared to anti- TNFα naïve patients, according to a greater expression of α4β7 integrin on vesicles surface. Circulating exosomes could compete for VDZ binding with CD4+ T cells since we found that the amount of VDZ bound to T cells was impaired in the presence of exosomes. In addition, we demonstrated that exosomes bind VDZ, which consequently becomes unable to block MadCAM-1-mediated adhesion of lymphocytes. Circulating exosomes might contribute to drug sequestration, possibly affecting the therapeutic efficacy of VDZ in IBD patients. Our data suggest that previous biologic therapy may have altered the sequestration capacity of circulating exosomes, thus reducing the efficacy of VDZ in patients who failed anti-TNF agents.https://doi.org/10.1371/journal.pone.0242342
collection DOAJ
language English
format Article
sources DOAJ
author Rossana Domenis
Marco Marino
Adriana Cifù
Giulia Scardino
Francesco Curcio
Martina Fabris
spellingShingle Rossana Domenis
Marco Marino
Adriana Cifù
Giulia Scardino
Francesco Curcio
Martina Fabris
Circulating exosomes express α4β7 integrin and compete with CD4+ T cells for the binding to Vedolizumab.
PLoS ONE
author_facet Rossana Domenis
Marco Marino
Adriana Cifù
Giulia Scardino
Francesco Curcio
Martina Fabris
author_sort Rossana Domenis
title Circulating exosomes express α4β7 integrin and compete with CD4+ T cells for the binding to Vedolizumab.
title_short Circulating exosomes express α4β7 integrin and compete with CD4+ T cells for the binding to Vedolizumab.
title_full Circulating exosomes express α4β7 integrin and compete with CD4+ T cells for the binding to Vedolizumab.
title_fullStr Circulating exosomes express α4β7 integrin and compete with CD4+ T cells for the binding to Vedolizumab.
title_full_unstemmed Circulating exosomes express α4β7 integrin and compete with CD4+ T cells for the binding to Vedolizumab.
title_sort circulating exosomes express α4β7 integrin and compete with cd4+ t cells for the binding to vedolizumab.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2020-01-01
description Vedolizumab (VDZ) is a therapeutic monoclonal antibody approved for the treatment of inflammatory bowel diseases (IBD). VDZ selectively binds to the α4β7 integrin and blocks trafficking of a specific subset of gastrointestinal-homing T-lymphocytes to inflamed tissue. Although VDZ has shown promising results in numerous clinical studies a subgroup of patients do not respond adequately. Mechanistic insights and prognostic biomarkers able to predict which patients might benefit from VDZ therapy are currently lacking. Circulating exosomes were isolated from serum of blood donors and VDZ-treated patients by polymer-based precipitation. The surface expression of α4β7 integrin was evaluated by flow cytometry and the levels of exosome-bound VDZ were investigated by Promonitor-VDZ ELISA kit. The capacity of exosomes to interfere with the adhesion of VDZ-treated CD4+ T cells was assessed by adhesion assay. In this study, we showed that serum exosomes isolated from both blood donor and ulcerative colitis patients express on their surface the VDZ target α4β7 integrin. We observed an increased exosomal sequestration of VDZ in anti-TNF exposed patients compared to anti- TNFα naïve patients, according to a greater expression of α4β7 integrin on vesicles surface. Circulating exosomes could compete for VDZ binding with CD4+ T cells since we found that the amount of VDZ bound to T cells was impaired in the presence of exosomes. In addition, we demonstrated that exosomes bind VDZ, which consequently becomes unable to block MadCAM-1-mediated adhesion of lymphocytes. Circulating exosomes might contribute to drug sequestration, possibly affecting the therapeutic efficacy of VDZ in IBD patients. Our data suggest that previous biologic therapy may have altered the sequestration capacity of circulating exosomes, thus reducing the efficacy of VDZ in patients who failed anti-TNF agents.
url https://doi.org/10.1371/journal.pone.0242342
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AT martinafabris circulatingexosomesexpressa4b7integrinandcompetewithcd4tcellsforthebindingtovedolizumab
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