STAT1 deficiency underlies a proinflammatory imprint of naive CD4+ T cells in spondyloarthritis

Bilade Cherqaoui; Bilade Cherqaoui; Frédéric Crémazy; Frédéric Crémazy; Marc Lauraine; Marc Lauraine; Ghazal Shammas; Ghazal Shammas; Roula Said-Nahal; Hendrick Mambu Mambueni; Hendrick Mambu Mambueni; Hendrick Mambu Mambueni; Félicie Costantino; Félicie Costantino; Félicie Costantino; Marine Fourmont; Marine Fourmont; Audrey Hulot; Audrey Hulot; Henri-Jean Garchon; Henri-Jean Garchon; Henri-Jean Garchon; Simon Glatigny; Simon Glatigny; Luiza M. Araujo; Luiza M. Araujo; Maxime Breban; Maxime Breban; Maxime Breban

doi:10.3389/fimmu.2023.1227281

Frontiers in Immunology (Oct 2023)

STAT1 deficiency underlies a proinflammatory imprint of naive CD4+ T cells in spondyloarthritis

Bilade Cherqaoui,
Bilade Cherqaoui,
Frédéric Crémazy,
Frédéric Crémazy,
Marc Lauraine,
Marc Lauraine,
Ghazal Shammas,
Ghazal Shammas,
Roula Said-Nahal,
Hendrick Mambu Mambueni,
Hendrick Mambu Mambueni,
Hendrick Mambu Mambueni,
Félicie Costantino,
Félicie Costantino,
Félicie Costantino,
Marine Fourmont,
Marine Fourmont,
Audrey Hulot,
Audrey Hulot,
Henri-Jean Garchon,
Henri-Jean Garchon,
Henri-Jean Garchon,
Simon Glatigny,
Simon Glatigny,
Luiza M. Araujo,
Luiza M. Araujo,
Maxime Breban,
Maxime Breban,
Maxime Breban

Affiliations

Bilade Cherqaoui: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Bilade Cherqaoui: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Frédéric Crémazy: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Frédéric Crémazy: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Marc Lauraine: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Marc Lauraine: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Ghazal Shammas: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Ghazal Shammas: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Roula Said-Nahal: Rheumatology Division, Ambroise Paré Hospital, AP-HP, Boulogne-Billancourt, France
Hendrick Mambu Mambueni: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Hendrick Mambu Mambueni: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Hendrick Mambu Mambueni: Genomic Platform of Faculty of Health Simone Veil, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Félicie Costantino: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Félicie Costantino: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Félicie Costantino: Rheumatology Division, Ambroise Paré Hospital, AP-HP, Boulogne-Billancourt, France
Marine Fourmont: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Marine Fourmont: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Audrey Hulot: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Audrey Hulot: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Henri-Jean Garchon: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Henri-Jean Garchon: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Henri-Jean Garchon: Genomic Platform of Faculty of Health Simone Veil, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Simon Glatigny: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Simon Glatigny: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Luiza M. Araujo: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Luiza M. Araujo: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Maxime Breban: Infection & Inflammation, UMR 1173, Inserm, UVSQ/Université Paris Saclay, Montigny-le-Bretonneux, France
Maxime Breban: Laboratoire d’Excellence Inflamex, Université Paris-Centre, Paris, France
Maxime Breban: Rheumatology Division, Ambroise Paré Hospital, AP-HP, Boulogne-Billancourt, France

DOI: https://doi.org/10.3389/fimmu.2023.1227281
Journal volume & issue: Vol. 14

Abstract

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IntroductionIn spondyloarthritis (SpA), an increased type 3 immune response, including T helper cells (Th) 17 excess, is observed in both human and SpA animal models, such as the HLA-B27/human β2-microglobulin transgenic rat (B27-rat).MethodsTo investigate this unexplained Th17-biased differentiation, we focused on understanding the immunobiology of B27-rat naive CD4+ T cells (Tn). ResultsWe observed that neutrally stimulated B27-rat Tn developed heightened Th17 profile even before disease onset, suggesting an intrinsic proinflammatory predisposition. In parallel with this observation, transcriptomic and epigenomic analyses showed that B27-rat Tn exhibited a decreased expression of Interferon/Th1- and increased expression of Th17-related genes. This molecular signature was predicted to be related to an imbalance of STAT1/STAT3 transcription factors activity. Stat1 mRNA and STAT1 protein expression were decreased before disease onset in Tn, even in their thymic precursors, whereas Stat3/STAT3 expression increased upon disease establishment. Confirming the relevance of these results, STAT1 mRNA expression was also decreased in Tn from SpA patients, as compared with healthy controls and rheumatoid arthritis patients. Finally, stimulation of B27-rat Tn with a selective STAT1 activator abolished this preferential IL-17A expression, suggesting that STAT1-altered activity in B27-rats allows Th17 differentiation. DiscussionAltogether, B27-rat Tn harbor a STAT1 deficiency preceding disease onset, which may occur during their thymic differentiation, secondarily associated with a persistent Th17 bias, which is imprinted at the epigenomic level. This early molecular phenomenon might lead to the persistent proinflammatory skew of CD4+ T cells in SpA patients, thus offering new clues to better understand and treat SpA.

Published in Frontiers in Immunology

ISSN: 1664-3224 (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: http://journal.frontiersin.org/journal/immunology

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