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INSERM researchers

RESTORE IMMUNE TOLERANCE IN RHEUMATOID ARTHRITIS

Pascale
LOUIS-PLENCE

Leader

Contact information
Phone: +33 4 67 33 57 21
email: pascale.plence@inserm.fr
Members

LOUIS-PLENCE Pascale (CRHC, INSERM), ORCID

SHAH Nainisha (PhD UM)

LAMBOUR Jennifer (Post-Doc, Arthritis4Cure)

NARBEBURU Emma (IE, Arthritis4Cure)


Members of ECELLFRANCE
Immunomonitoring platform

AFONSO Georgia (IE, UM), 

DUFOURCQ-LOPEZ Emilie (TCN, CHU)

Keywords

Immunotherapy

Dendritic cells

Treg lymphocytes

Tolerance

Arthritis

Rheumatoid arthritis

Immunomonitoring

Know how

Experimental Arthritis mouse models with clinical and immune monitoring

Phenotypic and functional characterization of DC and Treg subsets

Immunomonitoring of patients treated by biotherapies

Dendritic cell and Treg differentiation

The research aims of my group is focusing on:

  1. Development of novel and effective immunotherapeutic tools in Rheumatoid Arthritis
  2. Elucidating the role of DCs and/or regulatory cells in physiological and pathological conditions.
  3. Identifying biomarkers of response to biotherapies.

Restore immune tolerance without inducing global immune suppression using innovative antigen (Ag)-specific therapeutic molecule is the main issue of the CURE RA consortium (2018-2022), a collaborative project between 4 academic teams and the Arthritis R&D company. As a proof of concept, we demonstrated during the last 5 years, that an innovative hybrid molecule composed with a recombinant Fc region of an Ab, “clicked” with a citrullinated peptide, is able to specifically eliminate anti-citrullinated protein antibodies (ACPA)-positive B cells in vitro and in vivo, using antibody-dependent cell-mediated cytotoxicity (ADCC) and antibody-dependent cellular phagocytosis (ADCP) mechanisms. These unpublished results allowed us to deposit 3 patents. This innovative approach makes it possible to eliminate specific autoreactive ACPA+ B cells in RA patient. More importantly, our work opens up a new field of targeted treatment for systemic autoimmune diseases. However, the major limitation of our pilot study is that it showed in vitro and in vivo specific elimination of ACPA+ B cells and lacked substantial evidence to prove the therapeutic effects of the approach in vivo. The objective of the current project is to advance our understanding of the role of ACPA+ B cells in the pathophysiology of RA and to validate our therapeutic innovative approach to Cure RA. The 3 aims of the project are : 1-To address the safety of the therapeutic potential in immunocompetent mice. 2- To develop ACPA dependent experimental model of arthritis and evaluate the therapeutic potential of the elimination of ACPA+ B cell. 3- To determine the efficiency and specificity of the therapeutic approach in humanized mice model 

Main achievements:

  1. Immune tolerance induction using DC vaccination or adoptive Treg cell therapy
    https://doi.org/10.4049/JIMMUNOL.1501069
    https://doi.org/10.1186/AR4567
  2. Induction of Treg cells in patients treated by biotherapies
    https://doi.org/10.1002/ART.38246
    https://doi.org/10.7150/THNO.27674
  3. Characterization of Myeloid cells in synovial fluid from JIA patients
    https://www.frontiersin.org/articles/10.3389/fimmu.2020.01716/full