Arthritis, Rheumatoid Clinical Trial
Official title:
Characterization of the Effect of Tocilizumab in Vivo and in Vitro on T Follicular Helper Cells in Rheumatoid Arthritis Patients and Consequence on B Cells Maturation
Naïve CD4+ helper T (Th) cells, upon encountering their cognate antigens presented on
professional antigen-presenting cells, differentiate into different effector cells:
- Th1 cells produce Interferon-γ and regulate antigen presentation and immunity against
intracellular pathogens;
- Th2 cells produce IL-4 (Interleukin-4), IL-5 and IL-13, and mediate humoral responses
and immunity against parasites;
- Th17 cells produce IL-17, IL-17F and IL-22 and regulate inflammatory responses by tissue
cells.
An additional TH subset called follicular helper T (Tfh) cells has recently been identified
in germinal centers and also in whole blood (circulating Tfh cells). These cells regulate
B-cell maturation and immunoglobulin production during normal immune responses. They produce
factors essential for B cell selection and maturation into memory B-cells or long-lived
antibody-secreting plasma cells. Furthermore, they also seem to favor pathogenic autoantibody
production in systemic autoimmunity, and therefore could potentially represent a novel
therapeutic target in autoimmune diseases. Indeed, rheumatoid arthritis synovium is
characterized by the presence of ectopic lymphoid structures, resembling germinal centers.
Potentially, Tfh cells from these nonlymphoid tissues could promote B-cell maturation and
synthesis of pathogenic autoantibody production, thus potentiating tissue injury.
Interestingly, production of IL-21 by Tfh cells is implicated in B cell activation, and the
same cytokine have been associated with rheumatoid arthritis (RA) pathogenesis.
IL-6 blocking therapy significantly reduces signs and symptoms as well as radiological
progression in RA. However, so far, it has not been determined which of the pleiotropic IL-6
effects impact the observed clinical response. Recently, Samson et al have demonstrated that
Tocilizumab (TCZ) corrects the imbalance between Th17 cells and Treg cells in patients with
RA. More interestingly, the group of Hans-Peter Tony has reported the impact of TCZ on B cell
compartment. They showed a significant reduction in the frequency of peripheral pre-switch
and post-switch memory B cells but also a reduction of serum immunoglobulin levels, that
could be the reflect of TCZ on Tfh cells development, circulation and/or function.
Most of the work studying the role of IL-6 on Tfh cells development has been performed in
mice. They showed that optimal Tfh cells formation requires IL-21 and IL-6, and that
cytokines alone are insufficient to drive Tfh cells differentiation.
To better understand the impact of IL-6 on human Tfh cells, the investigators would like to
conduct a prospective study in patients with active RA and investigated the effects of
blocking IL-6 with TCZ on circulating Tfh cells levels and Tfh cells subsets over a 12-week
study period. Furthermore, the impact of TCZ treatment on Tfh cells generation will be
explored in vitro.
n/a
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