av Amanda S för 6 årar sedan
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LFA-1 bind tightly to ICAM-1
diapedesis: lymphocyte leaves blood and enters lymph node and goes to T cell region where Das are
from T cell region, 2 possible directions
Binding: T cell Receptor+ CD3+ CD4+ CD28 (co receptor binds to C7)
CD3, CD4, CD28 binding MHC molecule + peptide
SMAC T cell synapse
signals produced by CD4 to activate Lck
once interaction occurs, Lck is a kinase
LCK interacts with Zap70
phosphorylation of tyrosines CD3 group
NFAT
DAG
RAS
MAPK pathway
FOS
PCK-OMEGA
NFkB
No binding of TCR to MHC class II + peptide
has receptor for S-1-P moves to efferent lymphatic vessel
goes to next lymph node ends up in duct and blood stream where it can go to 2ndary lymphoid tissue
TCR complex
CD40L gets expressed on TFH and CD40L goes to CD40 on B cell
LFA-1 and ICAM synapse
TFH cytokines and cytokine receptors on B cells
Proliferation and differentiation of B cells then to either plasma, memory cells or migrate to 2ndary follicle in B cell zone
Migrate to 2ndary follicle
proliferation of B cells
centroblasts rapidly divide
centroblasts-->centrocytes in light zone along with FDC
these 2 interact due to AG on extension of FDC and BCR...affinity maturation occurring
competition between centrocytes to bind to antigen on FDCs...ones able to bind have highest affinity
BCR bind to antigen?
internalizes receptor mediated endocytosis
processing and presentation of MHC class II
move to T cell area, interacts with TFH cells (same as above with CD40 etc.)
can also bind to self antigen
energy and possible apoptosis
B7-CD28 monovalent binding of BCR
signals for survival for 1. return to GC 2. plasma cell using IL-10 to alumina propria, medulla cords or bone marrow 3. IL-4 to memory cell
Apoptosis
somatic hypermutation and isotope switching (AID) associated with dark zone of germinal center
Plasma cells: IL59, IL-6 come from TFH BLIMP-1-bell to stay in lymph node or bone marrow to plasma
Driven by Notch1
induces protease to cleave intracellular domain/release from plasma membrane. translocated to nucleus and turn on expression of genes for T cell development by removing repressive transcription factors
IL-7 receptor
double negative thymocyte (no CD4 OR CD8)
Notch1 rearrangement
rearrange Beta, gamma, delta
pre-T cell receptor (forms complex with CD3)
CD3 sends signals for proliferation (RAG 1 AND 2)
alpha chain rearrangement (gamma, delta)
Alpha:beta TCR--> MHC and self peptides
more alpha rearrangement if possible free Vs and Js still availalbe
back to MHC and self peptides
strong binding/moderate binding (best)
dendritic cells expressing AIRE (which turns on tissue specific genes) and macrophages
test for tissue specific self-peptides
cell dies
first allele, then second...still not productive then no further rearrangements
After D-->J then V-->DJ
large pre-B cell stage
lambda5 PreV
Mu combining with surrogate light chain and IgBeta/IgAlpha
signal sent that results in positive selection...survival
Rag1 and Rag2 stop being produced
proliferation/cell division
pre B cell stage and get light chain rearrangement starting...RAG1 and 2 expressed
production of IgM to surface by Igalpha and beta
sends signal to survive and RAG 1 and 2 not expressed
immature B lymphocyte
apoptosis
secrete CXCL13 (B cells move to FDCs)
FDC b-cell interaction
FDCs bind to LT produced by B cells to produce B-Aff
maturation and survival B cells (IgM/IgD)
encounters Ag on FDC
start of process B cell activation
BCR multiple receptor complex Igalpha and Igbeta and tryp
SYK binds adjacent IgB
LFA-1 on TFA bind ICAM-1 on B cell
synapse forms conjugate pair
END
antigen activated B cell
Move to B-T cell margin due to production of CCL219 by TFH bind CCR7
B cell internalize Ag through RME process and present peptide on MHC class II
Activated TFH
TFH more CD40 binds to CD40 on B cell
coreceptor Cd8+, CD19, CR2
CR2 binds iC3b
CD19 activated
CD19 phosphorylated by SYK
signal
encounters Ag away from FDC then Ag has C36 on surface
One of the J’s rearranges to one of the Ds anything between that DNA rearrangement gets lost.
Vh, Vh, Vh, Vh, Dh, Dh, Dh, Dh, Jh, Jh,
One the Ds can bind to the Vh variable too but everything between gets cut out
FADD/TRADD activate NFkappaB
NFkappa B causes synthesis and secretion of inflammatory cytokines
One site on MAVs engages TRAF6 which leads to activation of IRF3 and secretion of type 1 interferon.
Type 1 interferons (INFalpha and INFbeta) cause interferon response
3 major functions. 1. induce resistance to viral replication in all cells 2. increase expression of ligands for receptors on NK cells 3. Activate NK cells to kill virus-infected cells
C5b initiates the assembly of terminal complement to form membrane-attack complex
C5b, C6, C7 bind to pathogen surface. C8 and C7 undergo conformational change to expose hydrophobic sites...insert into membrane
induces polymerization of C9 to generate transmembrane channel
Factor H binds to C3b and changes conformation to cleavage by factor I
iC3b fragment of C3 remains attached to the pathogen surface but cannot form a c3 convertase
Properdin (factor P) binds to C3bB to extend its lifetime on microbial surface
C3a recruits phagocytic cells to site of infection
ip3 increases Ca2+-->activates calcineurin
NFAT activated
activates RasGRP, activates MAP kinase cascade
RAS-induced kinase induces and activates Fos
activated protein kinase C
activates NFkappaB
changes pattern of gene expression
CELL DIVISION, PROLIF., DIFFERENTIATION TO EFFECTOR T CELLS
any cell in bone marrow
immature B cell
if responds to self cells: either apoptosis or receptor editing
Positive selection
no receptor editing
immature to mature B cell
FDCs
postitive life signal; otherwise die in 3 days
2ndary lymphoid organ
B cell follice
negative selection
MHC present self antigen
lives
thymus, DC, Macrophages
receptor editing
Positive selection occurs in thymus
Recognize self MHC
dies
Lives
Beta chain
alpha chain
rearrange many times
DN4--> DP
2 on each chromosome
thymus
DN2
pTalpha
heavy chain
light chain
Immature B: do heavy/light chain produce functional binding site?
many rearrangements
small pre-b cell stage
Large preB--is chain functional?
early pre B to large pre B cell
Lambda5, VproB
2 (4 if counting DJ and VD seperate)
ACTIVATION of T cell
Process MHC class II
CD40L:CD40
IL-2 binds to IL-2R
Proliferation
2ndary lymphoid tissue
CD4 T cells
activate Macrophage and dendritic cells
need inflammatory response
Lymphoid tissues
T cell trafficking (4 steps)
diapedesis
chemokines
CCL21 & CXCL12
chemokine
CCL21
adhesion
integrins
LFA-1
Rolling
selection
L selection
APC
Clonal expansion
differentiation
cytokines
TYPES of what cell can turn into
TH1 activate macrophages help B cells produce Ab
CD8 cyto t cells kill infected cells
ways to activate CD8 cytotoxic T cells
Dendritic Cell
B7--> activate CD8
ADC
B7 & IL-2
CD4 T cell
IL-2
CD8 proliferation
TH2 parasitic/allergies help B cells produce Ab
TH17 enhance neutrophil response
TFH aid in isotype switching of B cells
TReg inhibits immature DCs
survival
CD28:B7
activation
MHC:TCR
present antigen
dendritic cell, macrophage
Thymus
Helper cells
cytotoxic T cells
Memory cells
Bone marrow
Activation Of B-cell
cross-link antigen
CR2
MHC class II
MHC class I
alpha 1 and 2
more than 10 AA
beta 1
CD40
alpha 1
CD3 on antigen
B cell
affinity maturation
Positively selected B cell
affinity for antigen
T cell help
B cell cross linking
plasma cells or memory cells
negatively selected B cell
APOPTOSIS
centroblasts
isotype switching
T cell
somatic hypermutation
point mutation
FDC's --> better selection
Centrocytes
germinal center
Memory B cell
Plasma cell
C1
C3bBb
C3bBb3b
C3b from other pathways
C4b2a3b
Mannose binding lectin
C4b2a