Rheumatoid Arthritis Clinical Trial
Official title:
Sequential B Cell/T Cell Therapy to Re-induce Humoral Immune TOLErance in ACPA- Positive Rheumatoid Arthritis A Prospective, Randomized Controlled Open Label Single-centre Clinical Trial in Adult Subjects With Active ACPA-positive Rheumatoid Arthritis Failing Methotrexate
Although anti-citrullinated protein antibodies (ACPA) including anti-CCP2 antibodies are known to promote inflammation and joint destruction in patients suffering from ACPA-positive rheumatoid arthritis, there are currently no therapies available to efficiently eliminate autoantibody production and to re-induce immune tolerance in these patients. However, both a B cell-targeting therapy (Rituximab) and a T cell targeting therapy (Abatacept) were described to lower anti-CCP2 antibody levels and occasionally trigger disappearance of these autoantibodies (sero conversion). By sequentially combining Rituximab and Abatacept, we thus aim to enhance the tolerogenic potential of these drugs and seek to eliminate autoantibody production and significantly lower ACPA titers. This would for the first time correspond to a "deep" immunological remission and a re-induction of immune tolerance.
Based on fact that both a B cell-targeting therapy with Rituximab and a T cell-targeting
therapy with Abatacept affect ACPA levels and can occasionally induce seroconversion and an
immunological remission as well immune tolerance in ACPA-positive RA patients, we conclude
that T/B cell-mediated autoimmunity can be in principle reversed in RA patients suffering
from active disease. We hypothesize that we can increase the tolerance-inducing potency of
Rituximab and Abatacept by combining these two approaches and delivering a sequential B
cell/T cell therapy with Rituximab and Abatacept. Such a combined approach might increase the
rate of seroconversions in RA patients and thus re-induce tolerance in a significant number
of patients which would pave the way for a long-lasting "deep immunological" and drug-free
remission.
In the proposed project, we thus plan to perform a sequential treatment with initial B cell
depletion with Rituximab followed by blockade of the immunological synapse by Abatacept. Such
an approach aims to deplete autoreactive B cells and plasmablasts, which constitute the major
source for ACPA (3) and thus reboot part of the immune system, before blocking the
immunological synapse in order to enable reconstitution of self-tolerance.
Based on their recently discovered pathogenic properties and to determine a potential
immunological remission in the participating RA patients, we primarily plan to evaluate the
effect of a sequential Rituximab/Abatacept treatment on changes in the levels of anti CCP2
antibodies between Baseline and Week 52 and will determine the rate of seroconversions.
Secondary, we plan to perform an additional quantitative and qualitative analysis of the ACPA
response. Glycosylation of ACPA was shown to modulate their inflammatory activity and is thus
considered to control the onset of arthritis in ACPA-positive individuals (9). We will
therefore measure glycosylation (galactosylation, fucosylation and sialylation) of ACPA and
total IgG. Moreover, we plan to determine changes in total IgG, IgA and IgM subclasses,
numbers of total B cells and plasmablasts as well as of CCP2-specific B cells and
plasmablasts in the peripheral blood of the participating patients. The clinical outcome will
be measured at week 52 described by disease activity parameters and patient questionnaires.
The longitudinal setup of this proof of concept mode of action study is to evaluate the
efficacy of a subsequent Abatacept therapy post B cell depletion in regard to ACPA
seroconversion, ACPA titers and B cell phenotype changes.
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