T-Cell Activation

Question 1

T- cell co stimulatory molecules in T-cell activation

Answer 1

CD4, CD28, CD2, LFA-1, CD40: (CD154)

Question 2

Dendritic cell co-stimulatory molecules in T-cell activation

Answer 2

HLA class II peptide, HLA class II, B7-1(CD80), B7-2(CD86), LFA-3, ICAM-1, ICAM-2, CD40

Question 3

Thp Activation

Answer 3

Expression of IL-2R, Secretion of IL-2, Autocrine and paracrine, clonal expansion of THP differentiation to TH0

Question 4

Th0

Answer 4

secretes IL-2, IL-4, IFN gamma,

Question 5

IL-2 is a growth factor for

Answer 5

T-cells

Question 6

IL-4 polarizes

Answer 6

response to TH2,

Question 7

IFN gamma polarizes

Answer 7

response to Th1

Question 8

IL-4 likely source is

Answer 8

mast cell

Question 9

IFN gamm source is

Answer 9

IL-12 activated NK cells.

Question 10

CTLA-4 is also known as

Answer 10

CD152

Question 11

CD152 has a higher affinity for

Answer 11

CD80 and CD86 than CD28

Question 12

CD200R is located on

Answer 12

Activated T-cells

Question 13

Signaling via CD200R is

Answer 13

inhibitory

Question 14

nTregs come from

Answer 14

thymic differentiation

Question 15

a/i Tregs differentiate from

Answer 15

Th0

Question 16

nTregs go after

Answer 16

self reactive T cells that have escaped negative selection

Question 17

both nTregs and a/i Tregs suppress

Answer 17

various immune responses

Question 18

IL-10 down regulates

Answer 18

secretion of IL-12 by dendritic cells

Question 19

IL-12 secreted by Dendritic cells affects

Answer 19

INF gamma secretion by NK cells and hence Th1 and Th1 cytokines

Question 20

nTregs contain

Answer 20

CD4+, CD25+, and FOXP3+

Question 21

nTregs also negatively control

Answer 21

immune responses to allo/non-self antigens

Question 22

Depletion of nTregs enhances

Answer 22

immune response to pathogens

Question 23

Depletion of nTregs leads to

Answer 23

tumor rejection

Question 24

Genetic mutations in FoxP3 result in

Answer 24

deficiency or dysfunction of Tregs

Question 25

Mutations Tregs=

Answer 25

disorder, IPEX (immune dysregulation, polyendocrinopathy, enteropathy, X-linked syndrome.

Question 26

a/i Tregs arise

Answer 26

in periphery following activation of Thp and Th0 cells

Question 27

a/i tRegs differentiation requires

Answer 27

TGF Beta

Question 28

Phenotype for a/i Tregs is

Answer 28

CD4+, CD25+, FOXP3+

Question 29

FOXP3 is a transcription factor that

Answer 29

is essentatil for development and function of regulatory T cells

Question 30

a/i Tregs control

Answer 30

immune response to both foreign and to self antigens by down regulating the function of effector CD4+ and effector CD8+

Question 31

three stages of Th17 differentiation

Answer 31

–differentiation which involves IL-1/IL6 and TGF Beta –stabilization(IL12 from dendritic cells and macrophages) –amplification (secreted by TH17 cells growth factor)

Question 32

Role in the immune response against extracellular pathogens not

Answer 32

eliminated by the CD4+ Th1 and CD4+ Th2 effector cells

Question 33

Th17 is effective in

Answer 33

eliminating fungal infections

Question 34

Th17 cells secrete

Answer 34

proinflammatory cytokines IL-17, IL-21, IL-22

Question 35

Th17 induce

Answer 35

the secretion of inflammatory mediators from macrophages and other cells that play a role in inflammation

Question 36

Inflammatory mediators include

Answer 36

various cytokines, chemokines and matrix metalloproteinases

Question 37

memory cells immunosurvey since they

Answer 37

have been presensitized to the immunizing agent that induced their differentiation

Question 38

re-exposure results in

Answer 38

secondary responses in a rapid 1-2 days

Question 39

conditions for memory T cell activation are

Answer 39

less stringent in requirements for adhesion and costimulatory molecules

Question 40

Antigen presenting cells (other than dendritic cells) can serve in

Answer 40

in the capacity of adhesion and costimulatory molecules early in response to antigen reexposure

Question 41

memory cell activation can occur at

Answer 41

the site of antigen contact, rather than in secondary lymphoid tissues.

Question 42

Memory CD4+ T cells secrete

Answer 42

cytokines.

Question 43

Type 2 Cytokines

Answer 43

IL-4,5,6,10,13 and TFG beta – they support B cell differentiation to plasma cells. –support isotype switching to IgG1 and IGE

Question 44

Thp cells differentiate to

Answer 44

Th1, Th2, a/iTregs, Th17

Question 45

activation of T-cells requires that the antigen

Answer 45

be displayed on the surface of an antigen presenting cell in association with Class II MHC

Question 46

the most effecient antigen presenting cell is

Answer 46

the dendritic cell.

Question 47

The antigen presenting dendritic cell expresses both

Answer 47

MHC class II and costimulatory molecules whose countermolecules are present on the T cell

Question 48

When a T cell interacts with peptide/MHC complexes in the absence of these costimulatory interactions then

Answer 48

the T cell becomes unresponsive

Question 49

ThP express receptors

Answer 49

IL-2 receptors and secrete the cytokine IL-2 that function in both autocrine and paracrine manner

Question 50

interaction with IL-2 and its receptors induces

Answer 50

clonal expansion of antigen stimulated T cells which increase the number of T cells with specificity uniquely recognizing the peptide/MHC class II complex that induced the initial differentiation

Question 51

critical signal in Tcell activation leading to clonal expansion is

Answer 51

CD28- CD80/86 interaction

Question 52

CD28-CD 80/86 interaction triggers

Answer 52

signal transduction events that lead to the stabilization of mRNA for IL-2

Question 53

Type 1 cytokines

Answer 53

IL-2 TNF, IFN gamma, support responses in which macrophages, NKC and CD8+tcells are effectors responsible for delayed type hypersensitivity responses that are manifestations of actibation of memory CD4+ Th1 cells. REQUIRED for immunity against viruses, parasites, fungi and intracellular bacteria

Question 54

Isotype switching requires contribution of

Answer 54

both type 1 and type 2 cytokines

Question 55

6 downregulators of T-cell activation

Answer 55

–elimination of infection –reciptorcal regulation (Th1 and Th2) – CTLA-4 CD152 interaction –CD200-CD200R interaction –apoptosis – Tregs

Question 56

CTLA-4 is not expressed

Answer 56

constitutively but peaks two days after the initial T cell activation and disappears by day 4

Question 57

CD200R is expressed primarily on

Answer 57

the cells of the myeloid lineage and on some T cells. 9higher on CD4 and higher on memory than naive.

Question 58

CD200R expression is upregulated on

Answer 58

both CD4+ and CD8+ after stimulation