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HLA-G may predict the disease course in patients
with early Rheumatoid Arthritis
Presented By: Nima Taefehshokr
MSc Biomedical Immunology
1
Human Immunology 74 (2013) 425-432
INTRODUCTION
• Rheumatoid Arthritis (RA) is an autoimmune inflammatory disease that is
characterized by synovitis leading to cartilage damage, bone erosion, joint
deformity and disability.
• Don’t forget the spinal cord.
• Both prevalence and incidence are 2-3 times
greater in women than in men.
• It affects approximately 1% population.
2
Key Factors
• Genetic: HLA-DR4 allels, PTPN22.
• Autoimmune: high titers of RF,
anti –CCP.
• Environmental: smoking, stress,
microorganisms.
• Endocrinologic: low levels of hormones from
the adrenal gland.
3
Pathogenesis of RA
• Intimal cell proliferation
• Inflammatory cell infiltration:T cells, B cells, macrophages and plasma cells.
• Production of cytokines and proteases.
• Increased vascularity.
• Self amplifying process.
4
BiologicalTherapeutics
Targets, Rationale, Status
5
Indian J Dermatol Venereol Leprol | September-October 2009 | Vol 75 | Issue 5
Reliable biomarker for ERA disease status
o HLA-G antigens are expressed as membrane bound and soluble
isoforms (mHLA-G , sHLA-G).
o These antigens are characterized as anti-inflammatory and
immunoinhibitory functions which act as ligand for ILT2, ILT4,
KIR2DL4.
o It has been reported that serum HLA-G concentration is significantly
lower in ERA patients.
o But, after DMARD (Disease-modifying Antirheumatic Drugs) therapy
there was a consistent up-modulation of HLA-G and ILT2.
6
Materials and methods
In this experiment 23 patients suffering from Early Arthritis met the criteria
to undergo DMARD therapy and were followed for 1 year.
o HLA-G polymorphism typing
o sHLA-G ELISA
o Cytokine plasma levels
o Cytometric analysis of PBMC
7
sHLA-G plasma levels
Figure.3 Increased levels of sHLA-G during 12 months therapy on the basis of DAS28 and
US-PD scores.
Cytokine plasma levels
Figure.4 (a) IL-1beta, IL-6,TNF –alpha,IL-10 plasma levels in Control subjects (HC),
ERA patients (ERA) and OArth subjects (OArth) before the therapy.
(b) IL-1 beta, IL-6,TNF-alpha,IL-10 levels during the 12 months follow-up disease
treatment.
9
Membrane HLA-G and ILT2 analysis by flow cytometry
(a) Increased expression of HLA-G and ILT2. (b) unmodified and slight increase of HLA-G,
ILT2 respectively. 10
Summery
• Low sHLA-G and mHLA-G expression suffered a more severe disease.
• DMARD therapy is able to modify HLA-G secretion.
• This confirmed the anti-inflammatory effect of DMARD by cytokine
evaluation that exerted its disease modifying effect partly by suppressing
Th1.
11
References
Rizzo, R., Farina, I., Bortolotti, D., Galuppi, E., Rotola,A
.,Melchiorri, L., Ciancio, G., Di-Luca, D. & Govoni,M.
2013. HLA-G may predict the disease course in patients with
early rheumatoid arthritis. Human Immunology. 74, 425-432.
12
13
Thank you.

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HLA-G may predict the disease course in patients with early Rheumatoid Arthritis

  • 1. HLA-G may predict the disease course in patients with early Rheumatoid Arthritis Presented By: Nima Taefehshokr MSc Biomedical Immunology 1 Human Immunology 74 (2013) 425-432
  • 2. INTRODUCTION • Rheumatoid Arthritis (RA) is an autoimmune inflammatory disease that is characterized by synovitis leading to cartilage damage, bone erosion, joint deformity and disability. • Don’t forget the spinal cord. • Both prevalence and incidence are 2-3 times greater in women than in men. • It affects approximately 1% population. 2
  • 3. Key Factors • Genetic: HLA-DR4 allels, PTPN22. • Autoimmune: high titers of RF, anti –CCP. • Environmental: smoking, stress, microorganisms. • Endocrinologic: low levels of hormones from the adrenal gland. 3
  • 4. Pathogenesis of RA • Intimal cell proliferation • Inflammatory cell infiltration:T cells, B cells, macrophages and plasma cells. • Production of cytokines and proteases. • Increased vascularity. • Self amplifying process. 4
  • 5. BiologicalTherapeutics Targets, Rationale, Status 5 Indian J Dermatol Venereol Leprol | September-October 2009 | Vol 75 | Issue 5
  • 6. Reliable biomarker for ERA disease status o HLA-G antigens are expressed as membrane bound and soluble isoforms (mHLA-G , sHLA-G). o These antigens are characterized as anti-inflammatory and immunoinhibitory functions which act as ligand for ILT2, ILT4, KIR2DL4. o It has been reported that serum HLA-G concentration is significantly lower in ERA patients. o But, after DMARD (Disease-modifying Antirheumatic Drugs) therapy there was a consistent up-modulation of HLA-G and ILT2. 6
  • 7. Materials and methods In this experiment 23 patients suffering from Early Arthritis met the criteria to undergo DMARD therapy and were followed for 1 year. o HLA-G polymorphism typing o sHLA-G ELISA o Cytokine plasma levels o Cytometric analysis of PBMC 7
  • 8. sHLA-G plasma levels Figure.3 Increased levels of sHLA-G during 12 months therapy on the basis of DAS28 and US-PD scores.
  • 9. Cytokine plasma levels Figure.4 (a) IL-1beta, IL-6,TNF –alpha,IL-10 plasma levels in Control subjects (HC), ERA patients (ERA) and OArth subjects (OArth) before the therapy. (b) IL-1 beta, IL-6,TNF-alpha,IL-10 levels during the 12 months follow-up disease treatment. 9
  • 10. Membrane HLA-G and ILT2 analysis by flow cytometry (a) Increased expression of HLA-G and ILT2. (b) unmodified and slight increase of HLA-G, ILT2 respectively. 10
  • 11. Summery • Low sHLA-G and mHLA-G expression suffered a more severe disease. • DMARD therapy is able to modify HLA-G secretion. • This confirmed the anti-inflammatory effect of DMARD by cytokine evaluation that exerted its disease modifying effect partly by suppressing Th1. 11
  • 12. References Rizzo, R., Farina, I., Bortolotti, D., Galuppi, E., Rotola,A .,Melchiorri, L., Ciancio, G., Di-Luca, D. & Govoni,M. 2013. HLA-G may predict the disease course in patients with early rheumatoid arthritis. Human Immunology. 74, 425-432. 12