IL-6-Driven PSTAT1 Response Is Linked to T Cell Features Implicated in Early Immune Dysregulation

Overview

Journal Front Immunol

Specialty Allergy & Immunology

Date 2022 Aug 1

PMID 35911690

Authors

Katharina Lambert

Kirsten E Diggins

Britta E Jones

Christian Hundhausen

Megan D Maerz

Anne M Hocking

Srinath Sanda

Carla J Greenbaum

Peter S Linsley

Karen Cerosaletti

Jane H Buckner

Affiliations

Soon will be listed here.

Abstract

Elevated levels and enhanced sensing of the pro-inflammatory cytokine interleukin-6 (IL-6) are key features of many autoimmune and inflammatory diseases. To better understand how IL-6 signaling may influence human T cell fate, we investigated the relationships between levels of components of the IL-6R complex, pSTAT responses, and transcriptomic and translational changes in CD4 and CD8 T cell subsets from healthy individuals after exposure to IL-6. Our findings highlight the striking heterogeneity in mbIL-6R and gp130 expression and IL-6-driven pSTAT1/3 responses across T cell subsets. Increased mbIL-6R expression correlated with enhanced signaling pSTAT1 with less impact on pSTAT3, most strikingly in CD4 naïve T cells. Additionally, IL-6 rapidly induced expression of transcription factors and surface receptors expressed by T follicular helper cells and altered expression of markers of apoptosis. Importantly, many of the features associated with the level of mbIL-6R expression on T cells were recapitulated both in the setting of tocilizumab therapy and when comparing donor CD4 T cells harboring the genetic variant, Asp358Ala (rs2228145), known to alter mbIL-6R expression on T cells. Collectively, these findings should be taken into account as we consider the role of IL-6 in disease pathogenesis and translating IL-6 biology into effective therapies for T cell-mediated autoimmune disease.

Citing Articles

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