Antigens

Question 1

What parts of pathogens does the adaptive immune system recognize?

Answer 1

Antigens.

Question 2

What is an antigen?

Answer 2

Any molecule that can interact with the immunoglobulin receptor of B-cells (or T-cell receptors complexed with MHC)

Question 3

What is an immunogen?

Answer 3

A molecule that induces a specific immune response.

Question 4

Are all immunogens antigens? Are all antigens immunogens?

Answer 4

Yes, no.

Question 5

Are immunogens and antigens universal, or are they context dependent?

Answer 5

Context dependent. Under different conditions, proteins can become antigens or immunogens.

Question 6

What is the order of immunogenicity for humoral immmunogens (B-cells)?

Answer 6

Proteins&raquo_space; Polysaccharides&raquo_space; Lipids & Nucleic Acids

Question 7

What is the order of immunogenicity for cell mediated immunogens (T-cells)?

Answer 7

Proteins (processed peptides in association with MHC molecules).

Question 8

What are the four properties of all immunogens?

Answer 8

Foreignness, molecular size, chemical heterogeneity, degradability.

Question 9

How does foreignness impact the strength of immunogens?

Answer 9

The degree of immunogenicity is dependent upon the degree of foreignness. The greater the phylogenetic distance between species, the greater the chance of immunogenicity (typically). Highly conserved regions may not be immunogenic, and some self molecules may raise an immune response in the animal they came from (sperm, lens tissue).

Question 10

How does molecular size impact the strength of immunogens?

Answer 10

Immunogens must be large enough to be processed.

Question 11

What is the ideal size of immunogens?

Answer 11

Approximately 100 000 Daltons.

Question 12

How does chemical heterogeneity contribute to the strength of immunogens?

Answer 12

Proteins with more complexity in primary structure, and those with secondary, tertiary, or quaternary structure show increased immunogenicity.

Question 13

How does degradability contribute to the strength of immunogens?

Answer 13

Proteins must be degraded to be presented by MHC molecules to activate T-cells. Insoluble molecules are more likely to be phagocytosed. Large molecules are processed more and have more epitopes. L-amino acids are better than D-amino acids as they are more easily processed.

Question 14

What are adjuvants?

Answer 14

Adjuvants are substances that, when injected with antigens, enhance the immunogenicity of the antigens.

Question 15

Are adjuvants specific to certain antigens?

Answer 15

No, they can be used with many different antigens.

Question 16

What are the three ways that adjuvants increase immunogenicity?

Answer 16

They stimulate an immune response, they prolong exposure to the antigen, and they release co-stimulatory signals.

Question 17

How do adjuvants stimulate an immune response?

Answer 17

Freund’s complete adjuvant, containing muramyl dipeptides from cell walls of heat killed mycobacteria, stimulates macrophage activity. This results in production of interleukin-1, which activates helper Tcells.

Question 18

How do adjuvants prolong exposure to the antigen?

Answer 18

Alum and Freund’s adjuvant bind and precipitate the antigen to keep it in the system longer, allowing for the slow release of the antigen. Precipitation also increases size of the antigen, facilitating phagocytosis.

Question 19

How do adjuvants produce a co-stimulatory signal?

Answer 19

Freund’s adjuvant and LPS upregulate co-stimulatory signal systems.

Question 20

What are epitopes?

Answer 20

Small, discrete sites on macromolecules that are recognized by lymphocytes (either B-cell or T-cell epitopes).

Question 21

How do B-cells bind to antigens?

Answer 21

Directly via cell surface immunoglobulins (lock and key fit)

Question 22

Can B-cell epitopes be nonsequential (conformational)?

Answer 22

Yes, B-cell epitopes can be sequential or nonsequential.

Question 23

What properties of epitopes are static for antigens in solution?

Answer 23

The epitopes must be topographically accessible on the native molecular surface (hydrophilic). The epitopes must also be flexible and mobile for agglutination (often located on bends and loop structure of protein).

Question 24

How big are linear epitope binding sites?

Answer 24

Typically 6-7 amino acids or sugars.

Question 25

How big are conformational epitope binding sites?

Answer 25

Typically 15-22 amino acids.

Question 26

Do all epitopes induce an immne response?

Answer 26

No, pathogens often make decoys that do nothing but are immunodominant to epitopes that are involved in pathogen function.

Question 27

What are conformational epitopes?

Answer 27

Any epitopes that are of secondary, tertiary, or quaternary protein structure.

Question 28

Do T-cells recognize soluble native antigens?

Answer 28

No.

Question 29

What types of antigens do T-cells recognize?

Answer 29

Those that have been processed and whose peptide fragments are presented in association with MHC molecules. (only linear epitopes)

Question 30

How big are T-cell epitopes?

Answer 30

Generally oligomeric peptides of 7-20 amino acids in size.

Question 31

How are antigens recognized by T-cells?

Answer 31

Antigens are seens as part of a trimolecular complex - T-cell receptor, antigen, and MHC.

Question 32

What properties must all antigens that activate T-cells have?

Answer 32

They must be amphipathic with a hydrophobic region that binds to MHC, and a hydrophilic region that binds to TCR

Question 33

What is the agretope?

Answer 33

The MHC binding site of the antigen that binds via hydrophobic amino acids.

Question 34

What is the T-cell receptor binding site that binds via hydrophilic amino acids called?

Answer 34

The epitope.

Question 35

Can the T-cell epitopes be internal pathogen proteins?

Answer 35

Yes. Since the pathogen must first be digested, both accessible and internal proteins may serve as epitopes for T-cells.

Question 36

Present in antigen-antibody interactions, what is reversible binding?

Answer 36

The molecules stick and fall off, stick and fall off, repeatedly.

Question 37

What type of bonds are responsible for antigen-antibody interactions?

Answer 37

Ionic bonds, hydrogen bonds, van der Waals interactions, hydrophobic bonds. NO COVALENT BONDS.

Question 38

What is affinity a measure of?

Answer 38

The sum total of non-covalent interactions between a single antigen binding site of antibodies and a single epitope. This is dictated by Ag/Ab fit.

Question 39

What is the formula for the association constant measuring affinity?

Answer 39

Ka = [Ab-Ag]/([Ab][Ag])

The concentration of antibody bound to antigen divided by the concentration of free antibody and free antigen.

Question 40

How is affinity experimentally measured?

Answer 40

Radiolabeled antigen is placed in a semi-permeable membrane that is impermeable to antibodies. A known concentration of antibodies are added to one side of the membrane. The concentration of free antigens will equillibrate on both sides of the membrane. The concentration of bound antigens/antibodies can be determined. This allows for the determination of free antibody concentration.

Question 41

What is avidity a measure of?

Answer 41

The stength of multiple interactions between multivalent antibody and antigen. This is dictated by affinity and the number of Ab/Ag bindings.

Question 42

How is avidity calculated from affinity?

Answer 42

Avidity = Affinity x # of binding sites.

Question 43

What are the two mechanisms of antigen cross-reactivity?

Answer 43

Different antigens may share common epitopes, allowing for one antibody to bind both antigens. The epitopes may be different but share common chemical properties. This also causes the antibody to bind two different epitopes.

Question 44

Describe how antigen cross-reactivity resulted in the ABO blood groups.

Answer 44

Anti-A antibodies originate from influenza virus, whose epitopes are similar to the A antigen. Anti-B antibodies result from glycoproteins on gram-negative bacteria (such as E. coli) that resemble B antigens.

Question 45

What is antigen precipitation?

Answer 45

When Ag-Ab interactions result in the formation of a lattice structure, forming precipitated antigen and antibody.

Question 46

What are the requirements of antigens and antibodies to form a lattice structure?

Answer 46

The antigen and antibody must be bivalent at least.

Question 47

When is maximal precipitation achieved?

Answer 47

In the Zone of Equivalence, when there is enough antigen and antibody without excess. This does not mean that the antibody and antigen concentrations need to be equivalent.