| Literature DB >> 32213704 |
Lauren A Henderson1, Kacie J Hoyt1, Pui Y Lee1,2, Deepak A Rao2, A Helena Jonsson2, Jennifer P Nguyen3, Kayleigh Rutherford4, Amélie M Julé1, Louis-Marie Charbonnier1, Siobhan Case1, Margaret H Chang1,2, Ezra M Cohen1, Fatma Dedeoglu1, Robert C Fuhlbrigge1,5, Olha Halyabar1, Melissa M Hazen1, Erin Janssen1, Susan Kim1, Jeffrey Lo1, Mindy S Lo1, Esra Meidan1, Mary Beth F Son1, Robert P Sundel1, Matthew L Stoll6, Chad Nusbaum7, James A Lederer3, Talal A Chatila1, Peter A Nigrovic1,2.
Abstract
Systemic juvenile idiopathic arthritis (sJIA) begins with fever, rash, and high-grade systemic inflammation but commonly progresses to a persistent afebrile arthritis. The basis for this transition is unknown. To evaluate a role for lymphocyte polarization, we characterized T cells from patients with acute and chronic sJIA using flow cytometry, mass cytometry, and RNA sequencing. Acute and chronic sJIA each featured an expanded population of activated Tregs uncommon in healthy controls or in children with nonsystemic JIA. In acute sJIA, Tregs expressed IL-17A and a gene expression signature reflecting Th17 polarization. In chronic sJIA, the Th17 transcriptional signature was identified in T effector cells (Teffs), although expression of IL-17A at the protein level remained rare. Th17 polarization was abrogated in patients responding to IL-1 blockade. These findings identify evolving Th17 polarization in sJIA that begins in Tregs and progresses to Teffs, likely reflecting the impact of the cytokine milieu and consistent with a biphasic model of disease pathogenesis. The results support T cells as a potential treatment target in sJIA.Entities:
Keywords: Autoimmune diseases; Autoimmunity; Inflammation; Rheumatology; T cells
Mesh:
Year: 2020 PMID: 32213704 PMCID: PMC7213804 DOI: 10.1172/jci.insight.132508
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708