Soluble antigen arrays disarm antigen-specific B cells to promote lasting immune tolerance in experimental autoimmune encephalomyelitis

Soluble antigen arrays disarm antigen-specific B cells to promote lasting immune tolerance in experimental autoimmune encephalomyelitis

Autoreactive lymphocytes that escape central immune tolerance may be silenced via an endogenous peripheral tolerance mechanism known as anergy. Antigen-specific therapies capable of inducing anergy may restore patients with autoimmune diseases to a healthy phenotype while avoiding deleterious side e...

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Veröffentlicht in:Journal of autoimmunity 2018-09, Vol.93, p.76-88
Hauptverfasser: Hartwell, Brittany L., Pickens, Chad J., Leon, Martin, Northrup, Laura, Christopher, Matthew A., Griffin, J. Daniel, Martinez-Becerra, Francisco, Berkland, Cory
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Antigen-specific B cells
Autoimmune-associated B cells
Autoimmunity
EAE
Tolerance
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container_end_page 88
container_issue
container_start_page 76
container_title Journal of autoimmunity
container_volume 93
creator Hartwell, Brittany L.
Pickens, Chad J.
Leon, Martin
Northrup, Laura
Christopher, Matthew A.
Griffin, J. Daniel
Martinez-Becerra, Francisco
Berkland, Cory
description Autoreactive lymphocytes that escape central immune tolerance may be silenced via an endogenous peripheral tolerance mechanism known as anergy. Antigen-specific therapies capable of inducing anergy may restore patients with autoimmune diseases to a healthy phenotype while avoiding deleterious side effects associated with global immunosuppression. Inducing anergy in B cells may be a particularly potent intervention, as B cells can contribute to autoimmune diseases through multiple mechanisms and offer the potential for direct antigen-specific targeting through the B cell receptor (BCR). Our previous results suggested autoreactive B cells may be silenced by multivalent ‘soluble antigen arrays’ (SAgAs), which are polymer conjugates displaying multiple copies of autoantigen with or without a secondary peptide that blocks intracellular cell-adhesion molecule-1 (ICAM-1). Here, key therapeutic molecular properties of SAgAs were identified and linked to the immunological mechanism through comprehensive cellular and in vivo analyses. We determined non-hydrolyzable ‘cSAgAs’ displaying multivalent ‘click’-conjugated antigen more potently suppressed experimental autoimmune encephalomyelitis (EAE) compared to hydrolyzable SAgAs capable of releasing conjugated antigen. cSAgAs restored a healthy phenotype in disease-specific antigen presenting cells (APCs) by inducing an anergic response in B cells and a subset of B cells called autoimmune-associated B cells (ABCs) that act as potent APCs in autoimmune disease. Accompanied by a cytokine response skewed towards a Th2/regulatory phenotype, this generated an environment of autoantigenic tolerance. By identifying key therapeutic molecular properties and an immunological mechanism that drives SAgA efficacy, this work guides the design of antigen-specific immunotherapies capable of inducing anergy. •Soluble antigen arrays (SAgAs) skewed B cells toward anergy to restore tolerance in a murine model of multiple sclerosis.•Therapeutic SAgA molecules consisted of multivalent autoantigen epitope linked to hyaluronan via non-degradable linker.•SAgAs exhibited disease-specific targeting of B cells and autoimmune-associated B cells through high avidity binding.•SAgAs caused downregulated costimulatory signaling in targeted B cells and shifted cytokines toward a regulatory response.•The SAgA mechanism was linked to molecular features to provide insight into the design of antigen-specific immunotherapies.
doi_str_mv 10.1016/j.jaut.2018.06.006
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Our previous results suggested autoreactive B cells may be silenced by multivalent ‘soluble antigen arrays’ (SAgAs), which are polymer conjugates displaying multiple copies of autoantigen with or without a secondary peptide that blocks intracellular cell-adhesion molecule-1 (ICAM-1). Here, key therapeutic molecular properties of SAgAs were identified and linked to the immunological mechanism through comprehensive cellular and in vivo analyses. We determined non-hydrolyzable ‘cSAgAs’ displaying multivalent ‘click’-conjugated antigen more potently suppressed experimental autoimmune encephalomyelitis (EAE) compared to hydrolyzable SAgAs capable of releasing conjugated antigen. cSAgAs restored a healthy phenotype in disease-specific antigen presenting cells (APCs) by inducing an anergic response in B cells and a subset of B cells called autoimmune-associated B cells (ABCs) that act as potent APCs in autoimmune disease. 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By identifying key therapeutic molecular properties and an immunological mechanism that drives SAgA efficacy, this work guides the design of antigen-specific immunotherapies capable of inducing anergy. •Soluble antigen arrays (SAgAs) skewed B cells toward anergy to restore tolerance in a murine model of multiple sclerosis.•Therapeutic SAgA molecules consisted of multivalent autoantigen epitope linked to hyaluronan via non-degradable linker.•SAgAs exhibited disease-specific targeting of B cells and autoimmune-associated B cells through high avidity binding.•SAgAs caused downregulated costimulatory signaling in targeted B cells and shifted cytokines toward a regulatory response.•The SAgA mechanism was linked to molecular features to provide insight into the design of antigen-specific immunotherapies.</description><identifier>ISSN: 0896-8411</identifier><identifier>EISSN: 1095-9157</identifier><identifier>DOI: 10.1016/j.jaut.2018.06.006</identifier><identifier>PMID: 30007842</identifier><language>eng</language><publisher>England: Elsevier Ltd</publisher><subject>Antigen-specific B cells ; Autoimmune-associated B cells ; Autoimmunity ; EAE ; Tolerance</subject><ispartof>Journal of autoimmunity, 2018-09, Vol.93, p.76-88</ispartof><rights>2018 Elsevier Ltd</rights><rights>Copyright © 2018 Elsevier Ltd. 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By identifying key therapeutic molecular properties and an immunological mechanism that drives SAgA efficacy, this work guides the design of antigen-specific immunotherapies capable of inducing anergy. •Soluble antigen arrays (SAgAs) skewed B cells toward anergy to restore tolerance in a murine model of multiple sclerosis.•Therapeutic SAgA molecules consisted of multivalent autoantigen epitope linked to hyaluronan via non-degradable linker.•SAgAs exhibited disease-specific targeting of B cells and autoimmune-associated B cells through high avidity binding.•SAgAs caused downregulated costimulatory signaling in targeted B cells and shifted cytokines toward a regulatory response.•The SAgA mechanism was linked to molecular features to provide insight into the design of antigen-specific immunotherapies.</description><subject>Antigen-specific B cells</subject><subject>Autoimmune-associated B cells</subject><subject>Autoimmunity</subject><subject>EAE</subject><subject>Tolerance</subject><issn>0896-8411</issn><issn>1095-9157</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2018</creationdate><recordtype>article</recordtype><recordid>eNp9UcuKFDEUDaI47egPuJD8QJU36UqqAiLo4AsGXKjrkEpu9aRJVYokPUx_gb9tmp4ZdOPqQs7jnptDyGsGLQMm3-7bvTmUlgMbWpAtgHxCNgyUaBQT_VOygUHJZugYuyAvct4DMCaEeE4utgDQDx3fkN8_YjiMAalZit_hQk1K5pip89mk-eG1yStaP3lLP1KLIWRaIl1TnGNBGkwuftlRP8-HBSsSMJnFIvULxbsVk59xKSbQGjbek7Di640JcT5i8MXnl-TZZELGV_fzkvz6_Onn1dfm-vuXb1cfrhvbCVEaPgjlhhGZGZ2ySk3W9Y7L0U68E6M10vRGgeqVxY4PsHW8Q96NnCvgbOJye0nen33XwzijszVZMkGvNaRJRx2N1_8ii7_Ru3irJWP9sFXVgJ8NbIo5J5wetQz0qRa916da9KkWDVLXWqrozd9bHyUPPVTCuzMB6-23HpPO1p8-yfmEtmgX_f_8_wD_0qSg</recordid><startdate>20180901</startdate><enddate>20180901</enddate><creator>Hartwell, Brittany L.</creator><creator>Pickens, Chad J.</creator><creator>Leon, Martin</creator><creator>Northrup, Laura</creator><creator>Christopher, Matthew A.</creator><creator>Griffin, J. 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subjects Antigen-specific B cells
Autoimmune-associated B cells
Autoimmunity
EAE
Tolerance
title Soluble antigen arrays disarm antigen-specific B cells to promote lasting immune tolerance in experimental autoimmune encephalomyelitis
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