Which pathogenic microbes can infect and life in host cells?
(1) Many bacteria, fungi, Protozoa can resist the killing mechanisms of these phagocytes.
(2) viruses that infect phagocytic and nonphagocytic cells.
Which T Lymphocyte is mainly responsible for for classical type of Cell-Mediated Immunity?
CD4+ T Cells
(CD8+ T Cells can eradicate infections without a requirement for phagocytes)
Steps of T-Cell mediated Immunity:
Types of effector CD4+ T cells:
Th1
Th2
Th17
Tfh(follicular helper cells)
What does the extracellular immune response against bacteria and fungi need to drive neutrophilic inflammation?
Cytokines
(All these types of Immune responses depend on CD4+ helper cells, they are able to stimulate distinct immune effector mechanisms)
Th1 Cells
stimulate phagocyte-mediated killing of ingested microbes
signature cytokine: interferon γ (IFN-γ) - most potent macrophage-activating cytokine
Acting through CD40L and IFN-γ increases ability of macrophages to kill phagocytosed microbes
Binding of CD40L to CD40 on macrophages functions together with IFN-γ binding to its receptor on same macrophage to trigger biochemical signaling pathways that lead to reactive oxygen species (ROS) and nitric oxide (NO) and activation of lysosomal proteases
Net result of CD40-mediated IFN-γ mediated activation: macrophages become strongly microbicidal and destroy most ingested microbes
How is the pathway of macrophage activation by CD40L and IFN-γ called?
Classic macrophage activation
M1 Macrophages (classically activated)
Also secrete cytokines that stimulate inflammation and express increased levels of MHC molecules and costimulators, which amplify T Cell response
Development of Th1 Cells
Driven by a combination of TCR signaling and cytokines IL-12 and IFN-γ
In response to many bacteria,viruses - dentritic cells and macrophages produce IL-12 and NK cells produce IFN-γ
T Cells are exposed to these cytokines if naive T cells recognize the antigens of these microbes
IL-12 and IFN-γ activate transcription factors Stat4 and Stat1
Antigen-induced signals in combination with cytokines induce expression of transcription factor T-bet (Th1 development and function)
These transcription factors stimulate expression of IFN-γ and other proteins involved in migration of Th1 cells to site of infection
IFN-γ activates not only macrophages, promotes also Th1 development and inhibits development of Th2 and Th17 cells
Th2 cells
induced by parasitic worm infections
Promote IgE-, mast cell- and eosinophil mediated destruction of these parasites
Signature cytokines: IL-4, IL-5 and IL-13
Principal target cells: Eosinophils
When Th2 and related Tfh cells encounter antigens of Helminths -> T cells secrete their cytokines
Tfh cells secrete IL-4 -> stimulates production of IgE antibodies
IgE antibodies coat Helminths and thus help in their clearance
Eosinophils use their Fc receptors to bind to IgE and are activated by IL-5 (produced by Th2)
Activated Eosinophils release their granules -> toxic to parasites
IL-13 stimulates mucus secretion and intestinal peristalsis -> increasing expulsion of parasites in intestines
IgE binds to mast cells and activates them -> secretion of chemical mediators that stimulate inflammation and proteases that destroy toxins
What is inhibited by Th2 cytokines?
Classical macrophage activation is inhibited
IL-4 and Il-13 inhibit classical
Alternative macrophage activation M2
activate macrophages to secrete growth factors (act on fibroblasts -> increase collagen synthesis + induce fibrosis
what kind of antigens can elicit also an Th2 response?
Allergens
allergens triggers mast cell and eosinophil activation
Development of Th2 Cells
differentiation of naive CD4+ T Cells to Th2 cells stimulated by IL-4 (produced by mast cells, other tissues)
IL4 activates transcription factor Stat6
Combo of IL4 and antigen-induced signals induce expression of GATA-3
GATA-3 -> required for Th2 differentiation
these TF stimulate expression of Th2 cytokines and promote Th2 response
IL-4 enhances further Th2 differentiation
Th17 Cells
Cytokines: IL-17, IL-22
Target Cells: Neutrophils
Host Defense: Extracellular fungi/bacteria
Functions of Cytokines:
IL-17
Stimulates chemokine secretion from other cells for leukocyte recruitment
Stimulates production of defensins (function like endogenous antibiotics)
Induce inflammation (prevent colonization, don’t kill, just pretend them from invading)
Stronger and longer inflammation response than in innate immunity
IL-22
Maintain integrity and repair damage of epithelial barriers
Development of Th17 cells
cytokines from macrophages and dendritic cells response to fungi and bacteria stimulate Th17 differentiantion
IL-1; IL-6 and IL-23 stimulate Stat3 (TF)
Signals induced by these inflammatory cytokines and transforming growth factor β (TGF-β) in combination with TCR signals -> expression of RORyT (TF)
TF are needed for differentiation of Th17
TGF-β is a powerful inhibitor of immune response but when present with IL-6 or IL-1 it promotes Th17 development
Development and functions of CD8+ T lymphocytes
CD8+ T cells recognize MHC 1 - antigen on an infected tissue cell and convert to CTLs (effected cells
Microbes in vesicles in cytosol, freely escaped in cytosol
Microbes captured by dendritic cells and then transferred to cytosol (Cross presentation)
Requires:
Antigen, Costimulation and help from CD4+ for activation
After activation no need for costimulation
Immune synapse:
TCR, CD8 signaling proteins cluster and becomes surrounded by LFA-1 Integrin -> bind to target cells
Release of granules
contain performing and granzymes into the synapse
Enter infected cells recognized by T lymphocyte and induce apoptosis
Fas Ligand on CTL bind to death inducing receptor Fas (CD95) on antigen -> apoptosis
Dead cells -> phagocytosed and eliminated, while CTLs can continue killing after detaching from cell
Functions of perforin
disrupt integrity of plasma and endosomal membranes -> delivery of granzymes to cytosol
Facilitates entry
Granzymes
Cleave and activate caspases -> induce apoptosis
What inhibits fusion of phagosomes/lysosomes
Myobacterium Tuberculosis
Legionella Pneumophilia
Listeria Monocytogenes
All inhibit fusion of phagosomes with lysosomes and escape into cytosol and thereby resist microbicial actions of phagosomes
What gets probably inhibited by certain viruses?
Production of Class 1 MHC molecules
Block of transport of antigenic peptides from cytosol to ER
Removes newly synthesized MHC from ER
-> reduces surface expression of MHC class 1 molecules
What can viruses produces to resist cell mediated immunity?
Inhibitory cytokines
Destroy cytokine receptors that would trigger cell mediated responses
Role of NK Cells
NK cells are activated by cells lacking MHC 1
This means that host Defense avoids immune evasion by microbes
CTLs recognizes MHC class 1 antigen peptides -> viruses inhibits MHC class molecules ->NK cells notices MHC1 deficency
T Cell exhaustion
Chronic infection by viruses that express inhibitory receptors such as PD-1 and
CTLA - 4 thus inhibiting the effector functions of CTLs
Zuletzt geändertvor 2 Jahren
