Abstract

Autoreactivity to AChR in the thymus of MG patientsMyasthenia Gravis (MG) is a disease caused by anti-acetylcholine receptor (AChR) autoantibodies. The thymus is clearly involved in the pathogenesis of MG: 50 percent of patients show thymic hyperplasia and 15 to 20 percent a thymoma; thymectomy is an efficient treatment for many patients. Our hypothesis is that the onset of MG disease with thymic hyperplasia is due to a coincidence of several components: the presence of the autoantigen, predisposition genes (namely MHC and cytokine genes) and a triggering event. In this favorable genetic situation, the triggering event could induce over activation of the immune system. Since AChR is present in the thymus and is highly immunogenic, and could be over expressed after the activation of the immune system, it could be efficiently presented. These events would lead to the formation of germinal centers and to production of anti-AChR antibodies inside the thymus. The long-term objectives of this application are to devise new approaches for treating MG disease. We must first understand the mechanisms underlying the induction of the anti-AChR autoimmune response in the thymus of MG patients.
The specific aims are to identify molecular and cellular components of the thymus that may be involved in inducing the anti-AChR autoimmune response and to create new models of thymic hyperplasia based on the data obtained. Several questions will be addressed: 1) Is the pattern of AChR expression normal in the thymic tissue of MG patients? Is AChR up regulated by mediators present in the thymus of MG patients? 2) Is the immune system dysregulated? Are the number and distribution of regulatory cells normal? 3) What are the phenotypic and functional characteristics of the autoreactive T cell clones isolated from the MG thymuses? 4) Where are the autoreactive B cells located in the thymus? and what are their frequencies? 5) What is the cascade of events leading to thymic hyperplasia? How to create an experimental model with thymic hyperplasia? The first 2 objectives will help to define the accurate state of the abnormalities in thymic hyperplasia; the objectives 3 and 4 will characterize the T and B cells involved in the pathogenesis and will be very helpful for defining new therapeutics. Finally if the components relevant for thymic hyperplasia are well defined, we should be able to create a new experimental model in which the pathophysiological role of these components will be directly evidenced and where the cascade of events leading to the thymic anti-AChR antibody production could be easily manipulated. Our project is original because we aim to study physiopathological mechanisms directly at the effector site using the relevant material. Patients with MG undergo thymectomy in our hospital. A large collection of pathological human tissue is available and represents an outstanding research material. Several methods will be used: quantitative autoradiography, quantitative RT-PCR, microarrays, transfection, digital image analysis, microdissection, flow cytometry, T cell clones, in situ hybridization, ELISA, alpha-bungarotoxin binding assays, SCID mice.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS039869-02
Application #
6529513
Study Section
Immunological Sciences Study Section (IMS)
Program Officer
Nichols, Paul L
Project Start
2001-09-24
Project End
2005-08-31
Budget Start
2002-09-01
Budget End
2003-08-31
Support Year
2
Fiscal Year
2002
Total Cost
$125,000
Indirect Cost

  Institution

Name
Hopital Marie Lannelongue
Department
Type
DUNS #
920150091
City
Le Plessis Robinson
State
Country
France
Zip Code
92350

  Publications

Gilboa-Geffen, Adi; Lacoste, Paul P; Soreq, Lilach et al. (2007) The thymic theme of acetylcholinesterase splice variants in myasthenia gravis. Blood 109:4383-91
Le Panse, Rozen; Cizeron-Clairac, Geraldine; Bismuth, Jacky et al. (2006) Microarrays reveal distinct gene signatures in the thymus of seropositive and seronegative myasthenia gravis patients and the role of CC chemokine ligand 21 in thymic hyperplasia. J Immunol 177:7868-79
Meraouna, Amel; Cizeron-Clairac, Geraldine; Panse, Rozen Le et al. (2006) The chemokine CXCL13 is a key molecule in autoimmune myasthenia gravis. Blood 108:432-40
Le Panse, R; Berrih-Aknin, S (2005) Thymic myoid cells protect thymocytes from apoptosis and modulate their differentiation: implication of the ERK and Akt signaling pathways. Cell Death Differ 12:463-72
Balandina, Anna; Lecart, Sandrine; Dartevelle, Philippe et al. (2005) Functional defect of regulatory CD4(+)CD25+ T cells in the thymus of patients with autoimmune myasthenia gravis. Blood 105:735-41
Nancy, Patrice; Berrih-Aknin, Sonia (2005) Differential estrogen receptor expression in autoimmune myasthenia gravis. Endocrinology 146:2345-53
Berrih-Aknin, Sonia; Fuchs, Sara; Souroujon, Miriam C (2005) Vaccines against myasthenia gravis. Expert Opin Biol Ther 5:983-95
Poea-Guyon, Sandrine; Christadoss, Premkumar; Le Panse, Rozen et al. (2005) Effects of cytokines on acetylcholine receptor expression: implications for myasthenia gravis. J Immunol 174:5941-9
Mesnard-Rouiller, Laurence; Bismuth, Jacky; Wakkach, Abdel et al. (2004) Thymic myoid cells express high levels of muscle genes. J Neuroimmunol 148:97-105
Balandina, A; Saoudi, A; Dartevelle, P et al. (2003) Analysis of CD4+CD25+ cell population in the thymus from myasthenia gravis patients. Ann N Y Acad Sci 998:275-7

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