Cell immune response

Question 1

Antigen presenting to naive t cells

Answer 1

T cell responses are initiated in the peripheral lymphoid organs, to which protein antigens are transported after being collected from their portal of entry

Dendritic cells that are resident in epithelia and tissues, capture protein antigens and transport them to draining lymph nodes

Question 2

DC properties that make them effective APC for primary T cell responses

Answer 2

DCs are strategically located at common sites of entry of microbes and in tissues that may be colonized by microbes
DCs express receptors that enable them to capture microbes and respond to microbes
They preferentially migrate to T-cell-rich zones of lymph nodes through which naive T-cells circulate
Mature DCs express high levels of co-stimulatory molecules, which are needed to activate naive T-cells
DCs can ingest infected cells and tumor cells and present antigens from these cells to CD8+ T cells

Question 3

Activation of T cells

Answer 3

Naive T cells circulate in secondary lymphoid organs
Native T cells acquire powerful functional capabilities only after they are activated
Antigen recognition by T cells leads to activation in form of:
-cytokin secretion
-proliferation (increase in the numbers of T cells of a specific clone)
-differentiation (of the naive cells into effector and memory T cells

Question 4

Naive T cells activated by:

Answer 4

Dendritic cells
DCs present peptides:
-from endocytosed protein antigens in association with class II MHC molecules to naive CD4+ T cells
-from cytosolic and nuclear proteins displayed by class I MHC molecules to CD8+ T cells

Question 5

Signals for T lymphocyte activation

Answer 5

Recognition of antigen is the first signal for the activation of T cells
CD4+ and CD8+ T cells recognize peptide-MHC complexes on APCs
Several other T cell surface proteins participate in the process of T cell activation

The second signal(s) for T cell activation is called costimulation
Signal 2 functions together with antigen (signal 1) to stimulate T cells

Question 6

Signal 2

Answer 6

CD28:B7 works in cooperation with antigen recognition to promote the survival, proliferation, and differentiation of the specific T cells

CD40L:CD40 interaction enhances T cell responses by activating the APCs (B7 expression on DCs)

Question 7

Regulation of T cell activation

Answer 7

T cell activation is influenced by a balance between engagement of activating and inhibitor receptors of the CD28 family
The inhibitory receptors of the CD28 family are CTLA-4 (cytotoxic T lymphocyte antigen 4) and PD-1 (programmed death 1)

CD28:B7 interaction is most important for initiating responses by activating naive T cells
ICOS:ICOS-ligand interactions are critical for helper T cell-dependent antibody responses
CTLA-4:B7 interactions inhibit the initial activation of T cells in secondary lymphoid organs
PD1:PD-ligand interactions inhibit the activation of effector cells in peripheral tissues

Question 8

Therapeutic costimulatory blockade

Answer 8

CTLA-4-Ig is an approved therapy for rheumatoid arthritis and transplant rejection
CTLA-4-Ig is in clinical trials for the treatment of psoriasis and crohns disease

Inhibitors of the CD40L:CD40 pathway are also in clinical trials for transplant rejection and chronic inflammatory diseases
Antibodies against CTLA-4 and PD-1 are approved or are in clinical trials for the immunotherapy of tumors

Question 9

Functional responses of T cell activation

Answer 9

Increase in surface molecule expression:

IL-2 secretion and IL-2Ra expression

Clonal expansion of T cells

Question 10

Functions of IL-2

Answer 10

Stimulates the survival, proliferation, and differentiation of antigen-activated T cells
Increases production of IFN-y and IL-4 by T cells
is required for the survival and function of regulatory T cells

Question 11

Therapeutic use of IL-2

Answer 11

Cancer

Canary pox virus

Question 12

Clonal expansion of T cells

Answer 12

Proliferation results in increase in number of the antigen specific clones-clonal expansion

Clonal expansion: production of daughter cells all arising originally from a single cell, In a clonal expansion of lymphocytes, all progeny \share the same antigen specificity

Before antigen exposure, the frequency of naive T cells specific for any antigen is 1 in 10^5 to 10^6 T cells
After antigen exposure the frequency of CD8+ T cell specific for that antigen increases to 1 in 3 CD8+ T cells and 1 in 100 CD4+ T cells

Question 13

Increase in surface molecule expression

Answer 13

CD69 (retention in lymph node), 
CD25 (IL-2Ra) (proliferation), 
CD40(activation of DCs, macrophages, B cells), 
CTLA-4 (Control of response), 
adhesion molecules, 
chemokine receptors

Question 14

IL-2 secretion and IL-2Ra expression

Answer 14

• IL-2 is a growth, survival, and differentiation factor for T cells
• it is produced mainly by CD4+ T cells early after antigen recognition and co-stimulation
• It acts on the same cells that produce it or on adjacent cells

Question 15

Differentiation of activated T cells into effector cells

Answer 15

Effector CD4+ cells express surface molecules and secrete cytokines that activate other cells (b lymphocytes, macrophages, and DCs)
Effector CD8+ cells are cytotoxic cells and kill infected cells

Question 16

Decline of T cell responses

Answer 16

Elimination of antigen leads to contraction of the T cell response
Decline is responsible for maintaining homeostasis in the immune system
Decline is due to:
-cessation of co-stimulation
-cessation of growth factor production (IL-2)
-activation of sensors of cellular stress (such as the BH3-only protein Bim), which triggers apoptosis of T cells

Question 17

Development of memory T cells

Answer 17

T-cell mediated immune responses to an antigen usually result in the generation of memory T cells specific for that antigen, which may persist for years, even a lifetime

Memory cells may develop from:

• effector cells along a linear pathway
• effector populations in divergent differentiation

Question 18

Properties of memory T cells

Answer 18

increases expression of anti-apoptotic proteins (Bcl-2 and Bcl-XL) responsible for their prolonged survival (long lived cells)
Respond more rapidly to antigen stimulation than naive cells specific for the same antigen
The number of memory T cells specific for any antigen is greater than the number of naive cells specific for the same antigen
Are able to migrate to peripheral tissues and respond to antigens at those sites
Undergo slow proliferation- self-renewal for prolonged lie span of the memory pool
Maintenance of memory cells is dependent on cytokines (IL-7) but does not require antigen recognition

Question 19

Role of CD4+ T cells in eradicating infections

Answer 19

Phagocytes with ingested microbes in vesicles
Cytokines secretion
Macrophages activation-> killing of ingested microbes
Inflammation, killing of microbes

Question 20

CD4+ T cells responses involve:

Answer 20

Initial activation in lymphoid organs

Generation of effector and memory cells

Migration of effector cells to sites of infection

Elimination of infectious pathogens at these sites

Functions of CD4+ T cells are mediated mainly by cytokines

CD4+ effector T cells are classifies according to the cytokines they produce

Question 21

Subsets of CD4+ Effector T cells

Answer 21

Three major subsets:
 Th1
Th2
Th17
follicular helper T cells

Question 22

Development of Th1, Th2, and Th17 subsets

Answer 22

All develop from naive CD4+ T lymphocytes
The development process is sometimes referred to as polarization of T cells
Process can be divided into:
-induction
-stable commitment
-amplification

Question 23

Th1 subset

Answer 23

Is induced by microbes that are ingested by phagocytes
Induced by microbes that activate phagocytes
Major effector T cell population in phagocyte-mediated host defense
The central reaction of cell-mediated immunity

Question 24

Development of Th1

Answer 24

Differentiate in the presence of IL-12 and IFN-y produced by DCs, macrophages, and NK cells

IFN-y and IL-12 stimulate Th1 differentiation bby activating the transcription factors T-bet, STAT1, and STAT4

IFN-y is produced and amplifies the development

Question 25

Functions of Th1 cells

Answer 25

Principal function of Th1 cells is to activate macrophages to ingest and destroy microbes

TH1 or follicular helper T cells stimulate the production of some IgG antibodies

Effector functions of Th1 cells are mediated through IFN-y

Question 26

Why if IFN-y important for Th1 celsl

Answer 26

It activates macrophages to kill phagocytosed microbes
It acts on B cells to promote IgG2a subclass switching and inhibits switching to IgE
It amplifies the Th1 subset and inhibits the development of Th2 and Th17 cells
It stimulates expression of molecules that enhance antigen presentation (e.g. increase MHC I and II)

Question 27

Therapeutic use of IFN-y in vetmed

Answer 27

Recombinant canine IFN-y (KT-100) in atopic dermatitis
hIFN-y against canine astrocytoma- clinical trials, gene therapy
fIFN-y in combination with fIL-2 and fGM-CSF- clinical trials fibrosarcoma, gene therapy
IFN-y gene therapy in canine brain tumors

Question 28

TH1-mediated classical macrophage activation and killing of phagocytosed microbes

Answer 28

Th1 cells activate macrophages by contact-mediated signals delivered by CD40L-CD40 interactions and by IFN-y

Responses of activated macrophages: enhanced killing of phagocytosed bacteria
secretion of inflammatory cytokines
Increased expression of molecules requires for T cell activation

Question 29

Th2 subset

Answer 29

Mediates phagocyte-independent defense

Eosinophils and mast cells play central roles in this defense

Important for the eradication of helminthic infections

Central to the development of allergic diseases

Question 30

Development of Th2 cells

Answer 30

Differentiation is stimulated by IL-4 in response to helminths and allergens

IL-4, IL-5 and IL-13 are the main Th2 cytokines

Question 31

Functions of Th2 cells

Answer 31

Stimulate:

• production of IgE
• mast cells
• eosinophils, these reactions eliminate helminthic infections
• alternative macrophage activation

Question 32

Classical macrophage activation

Answer 32

M1
Microbial TLR-ligands and IFN-y
-ROS, NO, lysosomal enzymes -> microbicidal actions: phagocytosis and killing of many bacteria and fungi
-IL-1, IL-12, IL-23, chemokines -> inflammation

Question 33

Alternative macrophage activation

Answer 33

M2
Monocyte, IL-13, IL-4

IL-10, TGF-B -> anti-inflammatory effects, wound repair, fibrosis

Question 34

Th17 subset

Answer 34

Responsible for recruiting leukocytes and inducing inflammation

• critical for destroying extracellular bacteria and fungi
• contribute to inflammatory diseases

Question 35

Development of Th17 cells

Answer 35

Stimulated by pro-inflammatory cytokines produced in response to bacteria and fungi

IL-1 and IL-6 initiate Th17 differentiation

IL-23 maintains proliferation and differentiation of Th17 cells

Question 36

Functions of Th17 cells

Answer 36

Combat microbes by recruiting neutrophils to sites of infection

They produce IL-17 which induces neutrophil-rich inflammation

IL-17 stimulates the production of antimicrobial substances

Question 37

Elimination of viruses by the immune system

Answer 37

Viruses cannot be destroyed by cells that lack microbicidal mechanisms

Viruses cannot be killed if they are in the cytosol where they are inaccessible to killing mechanisms

Ab neutralize before it enters cell- can be killed while inside cell

Kill the infected cell!

Question 38

Main function of CD8+ T cells

Answer 38

The function of killing cells with viruses in the cytosol is mediated by CD8+ cytotoxic T lymphocytes (CTLs)

Question 39

Other functions of CD8+ T cells

Answer 39

Eradication of tumors

Cytokine production

Critical roles in the acute rejection of organ allografts

Question 40

Differentiation of CD8+ T cells into cytotoxic T lymphocytes

Answer 40

Involves acquisition of the machinery to kill target cells

• acquisition of modified lysosomes- granules that contain perforin and granzymes
• acquisition of the capability to secrete cytokines, mostly IFN-y

Differentiation is controlled by 2 transcription factors, T-bet and oesmodermin

Question 41

Nature of antigen and antigen-presenting cells for activation of CD8+ T cells

Answer 41

Cytosol derived antigens can stimulate CD8+ T cells

Naive CD8+ T cells recognize antigen presented by MHC class I molecules on dendritic cells

Some APCs are not infected by the virus and do not endogenously synthesize viral antigen

• in such a situation the process of cross-presentation is used
• this process is also used to present tumor antigens
• only specialized subsets fo APCs can cross-present antigen (e.g. CD8+ DCs)

Question 42

Role of helper T cells in CD8+ T cell differentiation

Answer 42

Naive CD8+ T cells may require CD4+ T cell help to differentiate into functional CTLs and memory cells

• if APCs are directly infected by the microbe, CD4+ T cell help may not be critical
• CD4+ helper T cells may be required for CD8+ T cell responses to latent viral infections, organ transplants, and tumors

In weak innate immune reactions CD4+ T cell help if required

Question 43

Mechanisms of CD4+ T cell help to CD8+ CTLs differentiation

Answer 43

CD4+ helper T cells produce cytokines that stimulate CTL differentiation

CD4+ helper T cells enhance the ability of APCs to stimulate CTL differentiation

Question 44

Role of cytokines: IL-2

Answer 44

Promotes proliferation and differentiation of CD8+ T cells into effector CTLs and memory CTLs

Question 45

Role of cytokines: IL-12 and type I IFNs

Answer 45

stimulate the differentiation of naive CD8+ T cells into effector CTLs

Question 46

Role of cytokines: IL-15

Answer 46

Important for the survival of memory CD8+ T cells

Question 47

Role of cytokines: IL-21

Answer 47

Produced by activated CD4+ T cells induces CD8+ T cell memory

Question 48

Effector functions of CD8+ cytotoxic T cells

Answer 48

CD8+ CTLs eliminate intracellular microbes mainly by killing infected cells

CD8+ T cells secrete IFN-y

• contribute to classical macrophage activation in host defense
• stimulates hypersensitivity reactions

Question 49

Mechanisms of CTL-mediated cytotoxicity

Answer 49

CTL-mediated killing involves specific recognition of target cells and delivery of proteins that induce cell death

The process:

• antigen recognition (CD8 T cell has specific receptor for Ag; Ag presented by infected cell)
• activation of the CTLs
• delivery of the lethal hit that kills the target cells
• release of the CTLs

Question 50

Recognition of antigen and activation of CTLs

Answer 50

To be efficiently recognized by CTLs, target cells must:

• express class I MHC molecules complexed to a peptide
• binds to the CD8 co-receptor
• bind intercellular adhesion molecule 1 (ICAM-1, the principal ligand for the LFA-1 integrin)
• form an immunological synapse

Question 51

Two killing pathways

Answer 51

Perforin/granzyme-mediated cell killing

FAS/FASL-mediated cell killing

Question 52

Perforin/granzyme-mediated cell killing

Answer 52

The major cytotoxic proteins in the granules of CTLs (and NK cells) are granzyme B and perforin

Target cell and CD8+ CTL interact
CTL releases granule contents into immune synapses
Perforin induces uptake of granzymes into target cell endosome and release into cytosol, activating caspases
Perforates cell membrane
Apoptosis of target cell

Question 53

FAS/FASL-mediated cell killing

Answer 53

FasL on CTL interacts with Fas on target cell
Apoptosis of target cell

CTLs express a membrane protein called Fas ligand (FasL) that binds to the death receptor Fas, which is expressed on many cell types

Question 54

Inhibition of CD8+ T cell responses: the concept of T cell exhaustion

Answer 54

In some chronic viral infections, the responses of CD8+ T cells are initiated but gradually extinguished-phenomenon called exhaustion
Due to:
-reduced production of IFN-y
-increased expression of multiple inhibitory receptors e.g PD-1

Because they dont react they die

Question 55

Cytokine production by CD8+ Effector T cells

Answer 55

CD8+ T cells produce the macrophage-activating cytokine IFN-y

Question 56

Examples of chronic viral infections in animals

Answer 56

feline viral rhinotracheitis
feline calicivirus
canine distemper
feline leukemia