1. ANTIGEN-SPECIFIC T – CELL ACTIVATION MHC – peptide complex (ligand)
PARTNERS
Antigen presenting cell carrying antigenic peptides bound to MHC – pre-formed MHC – peptide complexes – INDEPENDENT ON T CELLS
Self MHC with captured antigenic peptide interacts with antigen-specific T lymphocytes selected from the available T cell repertoire
INTERACTION
MHC – peptide complex (ligand)
T cell receptor

2. MHC RESTRICTION
One single T-cell receptor can recognize a given MHC – peptid complex
If the peptide binds to another MHC molecule no T-cell recognition occurs
If the same MHC molecule binds another peptide, no T-cell recognition occurs

3. RECOGNITION OF CORRECT MHC – PEPTIDE COMPLEXES BY THE SPECIFIC T-CELL
Infected cell
Normal cell T
APC AND T CELL INTERACTION
IS IT SUFFICIENT FOR T CELL ACTIVATION?
WHERE AND WHEN CAN OCCUR?
HOW IS IT INDUCED?

4. VARIABILITY AND ORIENTATION OF CDR IN THE T CELL RECEPTOR
-chain
-CHAIN
Diszulfid hidak
CDR1 CDR CDR3
-chain
V C
CDR1 and CDR2 are not hypervariable
NO SOMATIC HYPERMUTATION
Variability of CDR3 is the result of joining variability
CDR1 CDR CDR3

5. INTERACTION OF THE T - CELL ANTIGEN RECEPTOR WITH AN MHC – PEPTIDE COMPLEX
TCR - MHC1
TCR - MHC1
CDR3 - peptide
The TCR is monovalent, binds a single MHC – peptide complex
The affinity of the TCR – peptide – MHC interaction is low M/l
A defined MHC – antigenic peptide complex is displayed in the cell membrane together with various other MHC – peptide complexes (DILUTED LIGAND)
How many MHC – peptide complexes are needed for T cell signaling?

6. THE IMMUNOLOGICAL SYNAPSE

7. THE IMMUNOLOGICAL SYNAPSE
ANTIGEN PRESENTING CELL
ICAM-1
LFA-1 B7
CD28
CD48
CD4
T CELL
CD2
SIGNALING COMPLEX
adaptor
ICAM – Intercellular Adhesion Molecule
ACTIVATED
T CELL

8. APC
T cell

9. THE INTERACTION OF T CELLS AND ANTIGEN PRESENTING CELLS
recognition 1 2 3 4 5 6 7 8
stabilization
separation
Negulescu P.A. et. al. Immunity 4: , 1996

10. THE CONTACT OF APC AND T CELLS IS STABILIZED BY ADHESION MOLECULES
MHCI – CD8
MHCII – CD4
CD40 – CD40L
B7 – CD28 *
B CELL
T CELL

11. KINETICS OF LYMPHOCYTE ACTIVATION
ANTIGEN
SIGNAL1.
Nyugvó limfocita G0
sejtosztódás
DNA synthesis
Effector cell Memory cell
Transport
Membrane change
RNA and protein synthesis
Resting lymphocyte G0
co-receptor
Adhesion molecule
Cytokines
SIGNAL2.
Resting lymphocyte G0
PTK activation RNA synthesis
Free Ca Protein synthesis
Protein phosphorylation DNA synthesis
Lymphoblast
0 10sec 1min 5min hr hrs hrs hrs

12. Similar but not identical signaling elements in B and T cells
BCR
TCR
Lyn
Kinases
Syk
Btk
fyn
ZAP70
Itk
SLP-65/BLNK
PLCg2
Adaptors +
substrates
PLCg1
SLP-76

13. T CELL RECEPTOR MEDIATED SIGNALING
Multisubunit Immune Recognition Receptors
MIRR
α β
ε δ ε γ
ζ ζ
ITAM
Immunoreceptor Tyrosine-based Activation Motif
ACTIVATION

14. TCR signaling
Fyn

15. Role of transcription factors in T-sejt activation

16. A T-sejt aktiválás intracelluláris folyamatai
INTRACELLULAR EVENTS OF T CELL ACTIVATION
A T-sejt aktiválás intracelluláris folyamatai
SIGNAL TRANSDUCTION
Enzimatic modification
(kinases, phosphatases, proteases)
Local concentration
(recruitment or
sequestration of interacting components
Timing
(pathway can go to diverse directions,
first one will be realized)
Allosteric effects
(binding activates or inactivates)
NEW GENES

17. INVOLVEMENT OF ADHESION AND CO-STIMULATORY MOLECULES
INTERACTION OF THE TCR WITH MHC-PEPTIDE COMPLEXES IS ESSENTIAL BUT NOT SUFFICIENT FOR T-CELL PRIMING
INVOLVEMENT OF ADHESION AND CO-STIMULATORY MOLECULES
CONVERGING SIGNALING PATHWAYS IN T CELL ACTIVATION
CD4/CD8 costimulation
CD28 costimulation

18. THE ADHESION AND CO-STIMULATORY MOLECULES CD4 AND CD8
MARKERS OF T CELL SUBPOPULATIONS
ADHESION MOLECULE
BINDS TO MHC
SIGNALING MOLECULE
TARGET CELL 1 3 2
2m 2 1 2 1
PROFESSIONAL APC
CD8
Cytotoxic T-cell
α β
Helper T-cell
CD4
SIGNAL

19. THE RATIO OF CD4+/CD8+ T CELLS IS STABLE IN HEALTHY INDIVIDUALS
Normal CD4+ T-cell counts = 600 – 1400/ l
HIV infection  AIDS = CD4+ T cell count <200/l