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Interferon-α-mediated therapeutic resistance in early rheumatoid arthritis implicates epigenetic reprogramming.
Cooles, Faye A H; Tarn, Jessica; Lendrem, Dennis W; Naamane, Najib; Lin, Chung Ma; Millar, Ben; Maney, Nicola J; Anderson, Amy E; Thalayasingam, Nishanthi; Diboll, Julie; Bondet, Vincent; Duffy, Darragh; Barnes, Michael R; Smith, Graham R; Ng, Sandra; Watson, David; Henkin, Rafael; Cope, Andrew P; Reynard, Louise N; Pratt, Arthur G; Isaacs, John D.
Afiliación
  • Cooles FAH; Translational and Clinical Research Institute, Newcastle University, Newcastle Upon Tyne, UK faye.cooles@ncl.ac.uk.
  • Tarn J; Translational and Clinical Research Institute, Newcastle University, Newcastle Upon Tyne, UK.
  • Lendrem DW; Translational and Clinical Research Institute, Newcastle University, Newcastle Upon Tyne, UK.
  • Naamane N; Translational and Clinical Research Institute, Newcastle University, Newcastle Upon Tyne, UK.
  • Lin CM; Translational and Clinical Research Institute, Newcastle University, Newcastle Upon Tyne, UK.
  • Millar B; Translational and Clinical Research Institute, Newcastle University, Newcastle Upon Tyne, UK.
  • Maney NJ; Translational and Clinical Research Institute, Newcastle University, Newcastle Upon Tyne, UK.
  • Anderson AE; Translational and Clinical Research Institute, Newcastle University, Newcastle Upon Tyne, UK.
  • Thalayasingam N; Translational and Clinical Research Institute, Newcastle University, Newcastle Upon Tyne, UK.
  • Diboll J; Translational and Clinical Research Institute, Newcastle University, Newcastle Upon Tyne, UK.
  • Bondet V; Laboratory of Dendritic Cell Immunobiology, Institut Pasteur, Paris, France.
  • Duffy D; Laboratory of Dendritic Cell Immunobiology, Institut Pasteur, Paris, France.
  • Barnes MR; Center for Translational Research, Institut Pasteur, Paris, France.
  • Smith GR; Centre for Translational Bioinformatics, William Harvey Research Institute, London, UK.
  • Ng S; Bioinformatics Support Unit, Newcastle University Faculty of Medical Sciences, Newcastle Upon Tyne, UK.
  • Watson D; Centre for Translational Bioinformatics, William Harvey Research Institute, London, UK.
  • Henkin R; Department of Statistical Science, University College London, London, UK.
  • Cope AP; Centre for Translational Bioinformatics, William Harvey Research Institute, London, UK.
  • Reynard LN; Academic Department of Rheumatology, King's College London, London, UK.
  • Pratt AG; Newcastle University Biosciences Institute, Newcastle University, Newcastle Upon Tyne, UK.
  • Isaacs JD; Musculoskeletal Research Group, The Freeman Hospital, Newcastle Upon Tyne, UK.
Ann Rheum Dis ; 2022 Jun 09.
Article en En | MEDLINE | ID: mdl-35680389
ABSTRACT

OBJECTIVES:

An interferon (IFN) gene signature (IGS) is present in approximately 50% of early, treatment naive rheumatoid arthritis (eRA) patients where it has been shown to negatively impact initial response to treatment. We wished to validate this effect and explore potential mechanisms of action.

METHODS:

In a multicentre inception cohort of eRA patients (n=191), we examined the whole blood IGS (MxA, IFI44L, OAS1, IFI6, ISG15) with reference to circulating IFN proteins, clinical outcomes and epigenetic influences on circulating CD19+ B and CD4+ T lymphocytes.

RESULTS:

We reproduced our previous findings demonstrating a raised baseline IGS. We additionally showed, for the first time, that the IGS in eRA reflects circulating IFN-α protein. Paired longitudinal analysis demonstrated a significant reduction between baseline and 6-month IGS and IFN-α levels (p<0.0001 for both). Despite this fall, a raised baseline IGS predicted worse 6-month clinical outcomes such as increased disease activity score (DAS-28, p=0.025) and lower likelihood of a good EULAR clinical response (p=0.034), which was independent of other conventional predictors of disease activity and clinical response. Molecular analysis of CD4+ T cells and CD19+ B cells demonstrated differentially methylated CPG sites and dysregulated expression of disease relevant genes, including PARP9, STAT1, and EPSTI1, associated with baseline IGS/IFNα levels. Differentially methylated CPG sites implicated altered transcription factor binding in B cells (GATA3, ETSI, NFATC2, EZH2) and T cells (p300, HIF1α).

CONCLUSIONS:

Our data suggest that, in eRA, IFN-α can cause a sustained, epigenetically mediated, pathogenic increase in lymphocyte activation and proliferation, and that the IGS is, therefore, a robust prognostic biomarker. Its persistent harmful effects provide a rationale for the initial therapeutic targeting of IFN-α in selected patients with eRA.
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Texto completo: 1 Colección: 01-internacional Base de datos: MEDLINE Tipo de estudio: Prognostic_studies Idioma: En Revista: Ann Rheum Dis Año: 2022 Tipo del documento: Article País de afiliación: Reino Unido
Texto completo
Añadir a Mi BVS
Imprimir
XML
PubMed Links
Buscar en Google

Texto completo: 1 Colección: 01-internacional Base de datos: MEDLINE Tipo de estudio: Prognostic_studies Idioma: En Revista: Ann Rheum Dis Año: 2022 Tipo del documento: Article País de afiliación: Reino Unido