Journal
RHEUMATOLOGY
Volume 49, Issue 1, Pages 156-166Publisher
OXFORD UNIV PRESS
DOI: 10.1093/rheumatology/kep345
Keywords
Type I interferon; Rheumatoid arthritis; Autoantibodies; Anti-citrullinated protein antibody
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Funding
- Netherlands Organization for Health Research and Development (ZonMw) [945-02-029]
- Reumafonds [NR 06-1303]
- Autocure
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Objective. Type I IFNs have recently been implicated in autoantibody-mediated diseases such as SLE. As half the RA patients display a type I IFN high signature, we investigated in a pilot study if type I IFN determines the autoantibody response in RA. Methods. Serum and peripheral blood cells were obtained from 52 RA patients, with paired samples before and after infliximab treatment in 21 patients. Additional samples were collected from 8 anti-citrullinated protein antibody (ACPA)-positive individuals without arthritis and from 10 ACPA-negative healthy controls. The type I IFN signature was determined by peripheral blood cell gene expression analysis and quantitative RT-PCR. ACPA IgG and IgM, RF IgM, anti-nucleosome IgM and anti-dsDNA were measured by ELISA. Results. The type I IFN signature was not related to the presence and titers of ACPA and RF during active disease. TNF blockade induced a similar rise of ANAs, and a similar decrease in RF titers in both groups. ACPA IgG and IgM levels appeared to be down-modulated only in the type I IFN low group. These changes were independent of the changes in type I IFN response gene activity after TNF blockade. Furthermore, the ACPA response in individuals without arthritis and inflammation was not related to an increase of type I IFN. Conclusions. In this explorative study, type I IFN signature does not appear to have a major impact on the humoral autoimmune response in RA. Replication of these data remains warranted.
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