MECHANISMS OF CELLULAR REJECTION IN ORGAN TRANSPLANTATION AN OVERVIEW

MECHANISMS OF CELLULAR REJECTION IN ORGAN TRANSPLANTATION AN OVERVIEW YVON LEBRANCHU Service Néphrologie et Immunologie Clinique CHU TOURS

ANTIGEN PRESENTING CELL CD4 + T CELL CYTOKINE PRODUCTION CLONAL EXPANSION ACTIVATED MACROPHAGES ACTIVATED B CELLS CD 8 T CELLS

WHERE DO T CELLS MEET TRANSPLANT ANTIGENS IN CONTEXT OF PLANNING AND INITIATING THE ALLO IMMUNE RESPONSE? DENDRITIC CELLS NAIVE T CELLS GRAFT SECONDARY LYMPHOID ORGANS

TWO POSSIBILITIES 2. RECIPIENT T LYMPHOCYTES RECOGNIZE ALLOGENEIC ANTIGENS PRESENTED BY GRAFT APC DENDRITIC CELLS NAIVE T CELLS GRAFT LYMPHOID ORGANS TWO POSSIBILITIES 1. GRAFT DENDRITIC CELLS MIGRATE TO SECONDARY LYMPHOID ORGANS DENDRITIC CELLS NAIVE T CELLS GRAFT LYMPHOID ORGANS

aly/aly (without lymph nodes and Peyer s patches) Hox 11 -/- (without spleen) HEART H-2 k Splenectomized aly/aly Control B6 Rôle essentiel des organes Lymphoïdes secondaires dans le rejet de Greffe de Coeur

GRAFT REJECTION Immature DC Graft Naive T cell activation Graft infiltration Naive T cell Mature DC Lymphoid organ MIGRATION DES CELLULES DENDRITIQUES CCR 5 CCR 7 LFA-1 VLA-4 CELLULE DENDRITIQUE IMMATURE CELLULE DENDRITIQUE MATURE

CD 4 T CELL ANTI DONOR RESPONSES INDIRECT DIRECT

GRAFT REJECTION Migration / Maturation Immature DC Graft Naive T cell Activation B cells Graft Infiltration Lymphoid organ Mature DC macrophage NK eosinophil Activated T cells THE 4 STAGES OF ACUTE REJECTION ALLO-ANTIGEN ANTIGEN RECOGNITION BY TCR T CELL ACTIVATION AND CLONAL PROLIFERATION GRAFT INFILTRATION PARENCHYMAL CELL DAMAGE

THE 4 STAGES OF ACUTE REJECTION ALLO-ANTIGEN ANTIGEN RECOGNITION BY TCR T CELL ACTIVATION AND CLONAL PROLIFERATION GRAFT INFILTRATION PARENCHYMAL CELL DAMAGE THE 4 STAGES OF ACUTE REJECTION ALLO-ANTIGEN ANTIGEN RECOGNITION BY TCR T CELL ACTIVATION AND CLONAL PROLIFERATION GRAFT INFILTRATION PARENCHYMAL CELL DAMAGE

T cell proliferation requires four different signals to induce allograft rejection Signal 1 (TCR engagement) and signal 2 (costimulation) to induce cytokine synthesis Signal 3 (IL-2) binding to its receptor) to induce cell cycle progression Signal 4 (nucleotide synthesis) to induce clonal T lymphocyte expansion

B 7 FAMILY 1. POSITIVE SIGNALS APC B 7.1 B 7.2 B 7.H B 7.H3 CD 28 ICOS? CD 4 T CELL

THE EXPANDING B 7 FAMILY LIGAND SIGNAL B 7.1 B 7.2 B 7 - H B 7 - H 3 CD 28 CD 28 ICOS? POSITIVE B 7.1 B 7.2 PD - L 1 PD - L 2 CTLA 4 CTLA 4 PD 1 PD 1 NEGATIVE Transduction signal (signal 3) is induced by IL-2 Binding to its receptor

IL-2 IL-15 M.TOR G 1 S

Nucleotide synthesis (signal 4) induces T cell proliferation This inhibitors of de novo nucleotide synthesis are immunosuppressive drugs THE 4 STAGES OF ACUTE REJECTION ALLO-ANTIGEN ANTIGEN RECOGNITION BY TCR T CELL ACTIVATION AND CLONAL PROLIFERATION GRAFT INFILTRATION PARENCHYMAL CELL DAMAGE

GRAFT REJECTION Immature DC Graft Naive T cell activation Graft infiltration Naive T cell Mature DC Lymphoid organ

CHEMOKINE RECEPTORS = SEVEN TRANSMEMBRANE RECEPTORS COUPLED TO G PROTEINS CXCR 1 to CXCR 5 XCR 1 Cx 3 CR 1 G PROTEIN CCR 1 to CCR 11 ONE CHEMOKINE CAN BIND TO SEVERAL RECEPTORS Rantes (CCL 5) bind to CCR 1, (mice), CCR 3, CCR 5 ONE CHEMOKINE RECEPTOR MAY TRANSDUCE SIGNALS FOR SEVERAL CHEMOKINES IP-10 (Cx CL 10), Mig (CxCL 9) and I-TAC (CxCL 11) bind to CXCR 3

THE 4 STAGES OF ACUTE REJECTION ALLO-ANTIGEN ANTIGEN RECOGNITION BY TCR T CELL ACTIVATION AND CLONAL PROLIFERATION GRAFT INFILTRATION PARENCHYMAL CELL DAMAGE

BUT, IN OTHER MODELS, MICE DEVOID OF PERIPHERAL LYMPHOID ORGANS CAN REJECT ALLOGENEIC GRAFTS. Lymphotoxin-α-deficient Lta - / -. Lymphotoxin-β-receptor deficient Ltbr - / - R. CHIN, P. ZHOU, M. ALEGRE and Y.X. FU Nature Med., 2001, 7 : 1165-1166

Rôle limité des organes lymphoïdes secondaires dans les rejets de greffe Peau Lta / Coeur Lta / splénectomisées SIGNIFICANCE? 1. REJECTION INDUCED BY GRAFT INFILTRATING MEMORY T CELLS? 2. DIRECT ALLORECOGNITION BY GRAFT ENDOTHELIAL CELLS?

SIGNIFICANCE? 1. REJECTION INDUCED BY GRAFT INFILTRATING MEMORY T CELLS? 2. DIRECT ALLORECOGNITION BY GRAFT ENDOTHELIAL CELLS? MHC CLASS I AND CLASS II MOLECULES AS WELL AS COSTIMULATORY MOLECULES ARE EXPRESSED ON VASCULAR ENDOTHELIUM, SPECIALLY UNDER INFLAMMATORY CONDITIONS IN VITRO STUDIES HAVE SHOWN THAT HUMAN T LYMPHOCYTES PROLIFERATE AFTER COCULTURE WITH VASCULAR ENDOTHELIAL CELLS BUT, IN VIVO?

ELEGANT TRANSGENIC ANIMAL MODEL BM3 T CELL RECEPTOR MICE (BACKGROUND CBA H-2 k ) RECOGNIZE A SINGLE ALLOGENEIC MHC CLASS I MOLECULE (H-2K b ) TWO NOVEL OBSERVATIONS 1. CD 8 + T CELLS CAN RECOGNIZE ALLO ANTIGENS ON GRAFT ENDOTHELIAL CELLS IN VITRO AND IN VIVO 2. T CELL-ENDOTHELIAL CELL INTERACTIONS, VIA DIRECT ALLORECOGNITION, CAN RESULT IN GRAFT REJECTION, EVEN IN THE ABSENCE OF CD4+ T CELLHELP AND PROFESSIONAL HEMATOPOIETIC ANTIGEN PRESENTING CELLS KREISEL, Nat. Med., 2002, 8 : 233-239

Rejet de greffe de cœur par CD8+ de souris BM3 déplétées en CD4+ B6 B6 (CBA) B6 (B6) infiltrat CD8+ CD4+ D. KREISEL Nature Médecine, 2002, 8 : 233-239 IN SUMMARY TWO PATHWAYS CLASSICAL PATHWAY = ACTIVATION OF ALLOGENEIC CD4 + T CELLS VIA DIRECT AND INDIRECT PATHWAYS IN SECONDARY LYMPHOID ORGANS ALTERNATIVE PATHWAY = DIRECT ALLOPRESENTATION BY ENDOTHELIUM TO CD8 + T CELLS, ESPECIALLY IN SITUATIONS WHERE CD4 + T CELL ACTIVATION HAS BEEN INHIBITED