Autoantibody-positive healthy individuals with lower lupus risk display a unique immune endotype

Autoimmune diseases comprise a spectrum of illnesses and are on the rise worldwide. Although antinuclear antibodies (ANAs) are detected in many autoimmune diseases, up to 20% of healthy women are ANA-positive (ANA+) and most will never develop clinical symptoms. Furthermore, disease transition is hi...

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Veröffentlicht in:Journal of allergy and clinical immunology 2020-12, Vol.146 (6), p.1419-1433
Hauptverfasser: Slight-Webb, Samantha, Smith, Miles, Bylinska, Aleksandra, Macwana, Susan, Guthridge, Carla, Lu, Rufei, Merrill, Joan T., Chakravarty, Eliza, Arriens, Cristina, Munroe, Melissa E., Maecker, Holden T., Utz, Paul J., Guthridge, Joel M., James, Judith A.
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container_end_page 1433
container_issue 6
container_start_page 1419
container_title Journal of allergy and clinical immunology
container_volume 146
creator Slight-Webb, Samantha
Smith, Miles
Bylinska, Aleksandra
Macwana, Susan
Guthridge, Carla
Lu, Rufei
Merrill, Joan T.
Chakravarty, Eliza
Arriens, Cristina
Munroe, Melissa E.
Maecker, Holden T.
Utz, Paul J.
Guthridge, Joel M.
James, Judith A.
description Autoimmune diseases comprise a spectrum of illnesses and are on the rise worldwide. Although antinuclear antibodies (ANAs) are detected in many autoimmune diseases, up to 20% of healthy women are ANA-positive (ANA+) and most will never develop clinical symptoms. Furthermore, disease transition is higher among ANA+ African Americans compared with ANA+ European Americans. We sought to determine the immune features that might define and prevent transition to clinical autoimmunity in ANA+ healthy individuals. We comprehensively phenotyped immune profiles of African Americans and European Americans who are ANA-negative (ANA−) healthy, ANA+ healthy, or have SLE using single cell mass cytometry, next-generation RNA-sequencing, multiplex cytokine profiling, and phospho-signaling analyses. We found that, compared with both ANA− and ANA+ healthy individuals, patients with SLE of both races displayed T-cell expansion and elevated expression of type I and II interferon pathways. We discovered a unique immune signature that suggests a suppressive immune phenotype and reduced CD11C+ autoimmunity-associated B cells in healthy ANA+ European Americans that is absent in their SLE or even healthy ANA− counterparts, or among African American cohorts. In contrast, ANA+ healthy African Americans exhibited elevated expression of T-cell activation markers and higher plasma levels of IL-6 than did healthy ANA+ European Americans. We propose that this novel immune signature identified in ANA+ healthy European Americans may protect them from T-cell expansion, heightened activation of interferon pathways, and disease transition. [Display omitted]
doi_str_mv 10.1016/j.jaci.2020.04.047
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Although antinuclear antibodies (ANAs) are detected in many autoimmune diseases, up to 20% of healthy women are ANA-positive (ANA+) and most will never develop clinical symptoms. Furthermore, disease transition is higher among ANA+ African Americans compared with ANA+ European Americans. We sought to determine the immune features that might define and prevent transition to clinical autoimmunity in ANA+ healthy individuals. We comprehensively phenotyped immune profiles of African Americans and European Americans who are ANA-negative (ANA−) healthy, ANA+ healthy, or have SLE using single cell mass cytometry, next-generation RNA-sequencing, multiplex cytokine profiling, and phospho-signaling analyses. We found that, compared with both ANA− and ANA+ healthy individuals, patients with SLE of both races displayed T-cell expansion and elevated expression of type I and II interferon pathways. We discovered a unique immune signature that suggests a suppressive immune phenotype and reduced CD11C+ autoimmunity-associated B cells in healthy ANA+ European Americans that is absent in their SLE or even healthy ANA− counterparts, or among African American cohorts. In contrast, ANA+ healthy African Americans exhibited elevated expression of T-cell activation markers and higher plasma levels of IL-6 than did healthy ANA+ European Americans. We propose that this novel immune signature identified in ANA+ healthy European Americans may protect them from T-cell expansion, heightened activation of interferon pathways, and disease transition. 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We discovered a unique immune signature that suggests a suppressive immune phenotype and reduced CD11C+ autoimmunity-associated B cells in healthy ANA+ European Americans that is absent in their SLE or even healthy ANA− counterparts, or among African American cohorts. In contrast, ANA+ healthy African Americans exhibited elevated expression of T-cell activation markers and higher plasma levels of IL-6 than did healthy ANA+ European Americans. We propose that this novel immune signature identified in ANA+ healthy European Americans may protect them from T-cell expansion, heightened activation of interferon pathways, and disease transition. 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subjects Adult
African Americans
ANA+ healthy
Antibodies, Antinuclear - immunology
Autoantibodies
cytokines
European Continental Ancestry Group
Female
Humans
immune suppression
Lupus Erythematosus, Systemic - immunology
Lupus Erythematosus, Systemic - pathology
Lymphocyte Activation
Male
race
Signal Transduction - immunology
SLE
T cells
T-Lymphocytes - immunology
T-Lymphocytes - pathology
title Autoantibody-positive healthy individuals with lower lupus risk display a unique immune endotype
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