Immunology: T cell development and Selection
Precursor T cell can go αβ, OR γδ TCR route
-Double negative T cells start to rearrange β, γ, and δ loci 1.γ and δ genes rearrange,γδ receptor assembles, stops further rearrangements > Matures into γδ cell 2. β rearranges, pre TCR assembles, signals through pre TCR stop rearrangment, induce expression of CD4 CD8, then cell rearrangement continues??
Describe the structure of the thymus
-STROMA of epithelial cells and CT -provides microenvironment of T cell development and selection -lobules split into outer cortex and inner medulla, filled with thymocytes form bone marrow -dendritic cells present
Peripheral tolerance
-T regulatory cells and regulatory receptors help tamp down T response when it gets too crazy and strong
T cell receptor: structure
-TWO chain heterodimer (α and β, OR γ and δ) -variable region, constant region, transmembrane region -CD3 help transport the signal
Genetic basis of TcR antigen-recognition diversity
-VJ and C regions rearrange like in the B cell and meet with different VJC regions (like α and β) -RAG enzymes randomly cut and recombine V,D,J -joints with N and P nucleotides
What are the CDRs?
-each TcR chain has 3 CDR's in variable region -hypervariable or complementarity determining region VARIABLE region actually contacts MHC
γδ T-cell
-emerge in waves during embryonic development -migrate to GI, pulmonary, and reproductive epithelium -response MUCH MORE rapidly than αβ (INNATE like) -bind to self MHC and MHC like molecules (like CD1 which recognizes lipids), recognize non protein antigens from important microbial patterns!!!!!
Autoimmunity implications
-if MHC making so many TCRs, then it is likely some will be matching to a self protein , lead to immune response against host
Auto immune regulator (AIRE)
-induces expression randomly by jumping around on genes and turning things on -epithelium can express things outside of thymus so exposure occurs
Central tolerance
-removal of self reactive T and B cells during development -T cell tolerance much more important than B cell tolerance since T cell needed to activate b cells
Self reactive T cells
-some antigens not present in thymus even with AIRE -some self peptides fail to form stable complexes on thymic stromal cells -failure of TcR to bind self peptide/MHC in thymus with sufficient avidity
What part of TcR actually reacts with peptide and self MHC?
-the variable region is what touches the MHC and the peptide
The Thymus
-where T cells undergo education -darker parts are rick in nuclei -atrophies with age
Cortex vs medulla of thymus
>Thymocytes, cortical epithelial cells, dendritic cells >Macrophage (eat up dead cells), medullary epithelial cell
Two classes of T cell receptors
>α chain and β chain , OR γ chain and δ chain
TcR development
HSC > Common lymphoid progenitor> migration from blood into thymus > T cell precursor > (double negative) DN1 (expressing certain factors) > DN2 > DN3 OR can change into γ δ cell > DN4 > Double positive (DP) > CD8+ or CD4+ then migrate out into periphery -90% alpha beta!
What determines αβ, OR γδ TCR ?
IF β rearranges first, it is αβ cell IF γδ rearranges, then γδ cell!
Do all T cells that mature in thymus come out?
No most die there -98% of them die without inflammation or change in size -thymic macrophages phagocytose apoptotic thymocytes
How does the T cell know if it will react with CD4 or CD8? Instructive model (in thymus)
Right now T cell is double positive! >If T cell receptor recognizes MHC class II, the CD4 its expressing will send signal (lose CD8) >if recognizes Class I, CD8 will saddle up to saddle chain, recognize it and signal T cell (lose CD4) Single positive thymocyte made
Negative selection
eliminate T cells that bind self MHC too tightly
Positive selection
reward T cells expressing TcR which can bind to self MHC
γδ T-cell go home to
specific epithelial tissues
Why do most cells die in thymus?
they are too useless or too dangerous >if too strong, leads to autoimmunity
Thymic atrophy
with age -however, still reasonably normal T cell bank when you are old
some autoimmune disorders
• TIDM • MS • Crohn's disease • Vitiligo • Rheumatoid arthritis • Hashimoto's disease
