Chapter 15 The adaptive Immune Response

Question 1

The scientist who received the first Nobel Prize in Medicine for his work on antibody therapy was

A. Koch.

B. von Behring.

C. Jenner.

D. Roux.

Answer 1

B. von Behring.

Question 2

Proteins that react specifically with the chemical structures in the antigen that induced them are called

A. determinants.

B. antibodies.

C. proteases.

D. macroproteins.

Answer 2

B. antibodies.

Question 3

Antibodies are made by

A. red blood cells.

B. macrophages.

C. B cells/plasma cells.

D. T cells.

Answer 3

C. B cells/plasma cells.

Question 4

T cells primarily are responsible for

A. humoral immunity.

B. cell-mediated immunity.

C. anamnestic immunity.

D. producing haptens.

Answer 4

B. cell-mediated immunity.

Question 5

Secondary lymphoid organs

A. are strategically located in the body.

B. facilitate interactions between cells.

C. are hematopoietic.

D. are the site of T cell maturation.

E. are strategically located in the body AND facilitate interactions between cells.

Answer 5

E. are strategically located in the body AND facilitate interactions between cells.

Question 6

Epitopes or antigenic determinants

A. are parts of the antibody molecule.

B. are T cell receptors.

C. are a portion of antigen recognized by antibody.

D. may be approximately 10-25 amino acids in length.

E. are a portion of antigen recognized by antibody AND may be approximately 10-25 amino acids in length.

Answer 6

E. are a portion of antigen recognized by antibody AND may be approximately 10-25 amino acids in length.

Question 7

The humoral immune response involves the manufacture and use of

A. antibodies.

B. T cells.

C. lymphokines.

D. antigens.

Answer 7

A. antibodies.

Question 8

Which of the following is not typical of an antigen?

A. low molecular weight

B. protein

C. foreign

D. polysaccharide

E. low molecular weight AND protein

Answer 8

A. low molecular weight

Question 9

Specific chemical groups on an antigen molecule to which the immune response is directed are

A. antigenic determinants.

B. an autoimmune response.

C. monomers.

D. allergens.

Answer 9

A. antigenic determinants.

Question 10

Generally antigenic molecules usually have a molecular weight greater than

A. 10,000 Daltons.

B. 100,000 Daltons.

C. glucose.

D. most polysaccharides.

Answer 10

A. 10,000 Daltons.

Question 11

Which of the following is/are secondary lymphoid organ(s)?

A. thymus

B. spleen

C. lymph nodes

D. bone marrow

E. spleen AND lymph nodes

Answer 11

E. spleen AND lymph nodes

Question 12

A term synonymous with antibody is

A. antigen.

B. epitope.

C. determinant.

D. immunoglobulin.

Answer 12

D. immunoglobulin.

Question 13

Which of the following do not induce a strong immune response?

A. lipids

B. proteins

C. polysaccharides

D. nucleic acids

E. lipids AND nucleic acids

Answer 13

E. lipids AND nucleic acids

Question 14

There are ______ classes of antibody.

A. 1

B. 3

C. 5

D. 7

Answer 14

C. 5

Question 15

Which of the following antibodies is a pentamer?

A. IgA

B. IgD

C. IgM

D. IgE

Answer 15

C. IgM

MASSIVE

Question 16

The chains of an antibody molecule are bonded to one another by

A. disulfide bonds.

B. hydrogen bonds.

C. ionic bonds.

D. oxygen bonds.

Answer 16

A. disulfide bonds.

Question 17

Which of the following antibodies is a dimer?

A. IgA

B. IgD

C. IgM

D. IgE

Answer 17

A. IgA

A plus you are a DIME

Question 18

The immunoglobulin monomer consists of

A. 4 large chains.

B. 2 heavy and 2 light chains.

C. 5 light chains.

D. 3 heavy and 3 light chains.

Answer 18

B. 2 heavy and 2 light chains.

Question 19

Which class of antibody accounts for the bulk of the circulating antibody?

A. IgA

B. IgD

C. IgG

D. IgE

Answer 19

C. IgG

Good Grief there are a lot

Question 20

The characteristic function and properties of each class of antibody is determined by the

A. variable region on the light chain.

B. epitope.

C. constant region on the light chain.

D. constant region on the heavy chain.

E. variable region on the heavy chain.

Answer 20

D. constant region on the heavy chain.

Question 21

An IgG molecule has two

A. heavy chains.

B. light chains.

C. antibody binding sites.

D. antigen binding sites.

E. heavy chains, light chains AND antigen binding sites.

Answer 21

E. heavy chains, light chains AND antigen binding sites.

Question 22

The variable region of an antibody occurs

A. only on the heavy chains.

B. only on the light chains.

C. on one of the light chains.

D. on all 4 chains.

Answer 22

D. on all 4 chains.

Question 23

Each class of antibody is specifically defined by its

A. amino acid sequence of the constant region of the heavy chain.

B. amino acid sequence of the variable region of the light chain.

C. ability to cross the placenta.

D. disulfide bonds.

Answer 23

A. amino acid sequence of the constant region of the heavy chain.

Question 24

Antigens interact with antibodies at

A. the outer end of each arm of the Y.

B. the junction of heavy and light chains.

C. different regions depending on the class of antibody.

D. the bottom stem of the heavy chain of the Y.

Answer 24

A. the outer end of each arm of the Y.

Question 25

Ag-Ab binding may result in

A. neutralization.

B. immobilization.

C. agglutination.

D. opsonization.

E. All of the choices are correct.

Answer 25

E. All of the choices are correct.

Question 26

The Fc region on IgG

A. interacts with complement.

B. attaches to receptors on interleukin-1.

C. reacts with and coats the antigen.

D. contains a variable region.

E. interacts with complement AND attaches to receptors on interleukin-1.

Answer 26

A. interacts with complement.

Question 27

How long after initiation of a primary response do significant amounts of antibody appear in the blood?

A. one day

B. 10-14 days

C. 4 weeks

D. 6 months

Answer 27

B. 10-14 days

Question 28

The only class of antibody that can cross the placenta is

A. IgA.

B. IgD.

C. IgG.

D. IgE.

Answer 28

C. IgG.

GOO GOO gaa gaa

Question 29

Which is the first antibody class made during the primary response to an antigen?

A. IgA

B. IgM

C. IgG

D. IgE

Answer 29

B. IgM

Question 30

Which of the following is the most abundant immunological class produced?

A. IgA

B. IgD

C. IgG

D. IgE

Answer 30

A. IgA

most produced but it leaves in mucus, tears, saliva etc.

AWAY

Question 31

Which is the most efficient at initiating the classical pathway of the complement cascade?

A. IgA

B. IgD

C. IgM

D. IgE

Answer 31

C. IgM

Question 32

Which of the following class of antibody is primarily found in external secretions?

A. IgA

B. IgD

C. IgG

D. IgE

Answer 32

A. IgA

AWAY

Question 33

The function of the secretory component of the IgA molecule is

A. to protect IgA from being destroyed by proteolytic enzymes.

B. to coat the antigen.

C. opsonization.

D. to fix IgA to the antigen.

Answer 33

A. to protect IgA from being destroyed by proteolytic enzymes.

Question 34

The immunoglobulin that is important in hypersensitivity reactions is

A. IgA.

B. IgD.

C. IgG.

D. IgE.

Answer 34

D. IgE.

Question 35

According to the clonal selection theory

A. antibodies are modified, at the time of antigen exposure, to specifically react with the antigen.

B. self-reactive T cells are killed in the thymus.

C. B cells producing autoantibodies are eliminated in the thymus.

D. each B cell is already programmed to produce a specific antibody.

E. self-reactive T cells are killed in the thymus AND B cells producing autoantibodies are eliminated in the thymus.

Answer 35

D. each B cell is already programmed to produce a specific antibody.

Question 36

“Clonal selection” and “clonal expansion”

A. implies that each individual lymphocyte produces a single antibody.

B. describes how the adaptive immune system can produce millions of different antibodies.

C. depends on an antibody recognizing a specific epitope.

D. are based on random processes.

E. All of the above

Answer 36

E. All of the above

Question 37

T cells and B cells are manufactured in the

A. bone marrow.

B. thymus.

C. Peyer’s patches.

D. nervous tissue.

Answer 37

A. bone marrow.

Question 38

T cells mature in the

A. bone marrow.

B. thymus.

C. Peyer’s patches.

D. nervous tissue.

Answer 38

B. thymus.

Question 39

The cells that actually secrete antibodies are

A. plasma cells.

B. natural killer cells.

C. phagocytes.

D. T cells.

Answer 39

A. plasma cells.

Question 40

CD4 cells are often

A. T helper cells.

B. T suppresser cells.

C. T cytotoxic cells.

D. T hypersensitivity cells.

Answer 40

A. T helper cells.

Question 41

CD8 cells are often

A. T helper cells.

B. T suppresser cells.

C. T cytotoxic cells.

D. T hypersensitivity cells.

Answer 41

C. T cytotoxic cells.

Question 42

Antigens may be processed for presentation by

A. macrophages.

B. dendritic cells.

C. erythrocytes.

D. T cytotoxic cells.

E. macrophages AND dendritic cells.

Answer 42

E. macrophages AND dendritic cells.

Question 43

Macrophages and dendritic cells are

A. T cells.

B. B cells.

C. antigen-presenting cells.

D. antibody-producing cells.

Answer 43

C. antigen-presenting cells.

Question 44

Only antigen-presenting cells

A. produce antibodies.

B. activate cytotoxic T cells.

C. produce MHC class I molecules.

D. produce MHC class II molecules.

Answer 44

D. produce MHC class II molecules.

Question 45

It would be useful if antigens were delivered directly to

A. Peyer’s patches.

B. W Cells.

C. M cells.

D. red blood cells.

E. Peyer’s patches AND M cells.

Answer 45

E. Peyer’s patches AND M cells.

Question 46

Class II MHC molecules are found primarily on

A. macrophages.

B. dendritic cells.

C. erythrocytes.

D. T cytotoxic cells.

E. macrophages AND dendritic cells.

Answer 46

E. macrophages AND dendritic cells.

Question 47

The stimulation of B cells to divide and mature is provided by

A. T helper cells.

B. macrophages.

C. T cytotoxic cells.

D. plasma cells.

Answer 47

A. T helper cells.

Question 48

The peptides presented by MHC class II peptide molecules are

A. from plasma cells.

B. exogenous antigens.

C. endogenous antigens.

D. from T helper cells.

Answer 48

B. exogenous antigens.

Question 49

T-independent antigens

A. include polysaccharides.

B. require the involvement of T cells.

C. interact with MHCI molecules.

D. are usually proteins.

E. include polysaccharides AND are usually proteins.

Answer 49

A. include polysaccharides.

Question 50

Memory cells may take the form of

A. B cells.

B. T cytotoxic cells.

C. T helper cells.

D. All of the choices are correct.

Answer 50

D. All of the choices are correct.

Question 51

The surface receptors on B and T cells both

A. play the same role in each type of cell.

B. bind to free antigen.

C. have two binding sites for antigen.

D. have variable and constant regions.

E. play the same role in each type of cell AND have two binding sites for antigen.

Answer 51

D. have variable and constant regions.

Question 52

Which is involved in reacting to virus-infected cells?

A. cell-mediated immunity

B. T cytotoxic cells

C. B cells

D. MHC I

E. cell-mediated immunity, T cytotoxic cells AND MHC I

Answer 52

E. cell-mediated immunity, T cytotoxic cells AND MHC I

Question 53

Perforin is produced by

A. B cells.

B. macrophages.

C. NK cells.

D. T helper cells.

E. macrophages AND NK cells.

Answer 53

C. NK cells.

Question 54

Giant cells are

A. a fusion of B cells.

B. a fusion of T cells.

C. used to contain bacterial infections.

D. activated T helper cells.

E. a fusion of T cells AND used to contain bacterial infections.

Answer 54

C. used to contain bacterial infections.

Question 55

Apoptosis

A. is a form of cell suicide.

B. is induced in target cells by effector T cytotoxic cells.

C. results in T cell death.

D. refers to the transformation of B cells into plasma cells.

E. is a form of cell suicide AND is induced in target cells by effector T cytotoxic cells.

Answer 55

E. is a form of cell suicide AND is induced in target cells by effector T cytotoxic cells.

Question 56

Substances with a molecular weight of less than 10,000 Daltons make good antigens

Answer 56

FALSE

Question 57

The immune response is directed against an entire molecule.

Answer 57

FALSE

Question 58

All antigens are immunogens.

Answer 58

FALSE

Question 59

Antibody molecules are very rigid in structure.

Answer 59

FALSE

Question 60

Antibody and antigen are held to one another by covalent bonds.

Answer 60

FALSE

Question 61

IgA is the most abundant immunoglobulin made by the body

Answer 61

TRUE

Question 62

Gene rearrangement is responsible for the generation of the various antibody molecules

Answer 62

TRUE

Question 63

T cells are responsible for directly manufacturing antibodies.

Answer 63

FALSE

Question 64

T cell receptors are identical to antibodies.

Answer 64

FALSE

Question 65

T cell independent antigens lead to a memory response.

Answer 65

FALSE

Question 66

How is the central portion of a T-cell receptor complex functionally analogous to the center of the B-cell receptor complex?

A. It has 2 pieces (chains), just like a B-cell receptor.

B. Both receptors bind epitopes (small amino acid sections of antigen molecules).

C. Both bind structures directly on the surface of microbes.

D. Both can be secreted from lymphocytes to bind to pathogens under certain situations.

Answer 66

B. Both receptors bind epitopes (small amino acid sections of antigen molecules).

Question 67

How is a T-cell receptor different from a B-cell receptor?

A. T-cell receptors must have antigen broken down inside a cell and presented to them by a Major Histocompatibility Complex (MHC) molecule.

B. B-cell receptors must have antigen broken down inside a cell and presented to them by a Major Histocompatibility Complex (MHC) molecule.

C. T-cell receptors are composed of 4 protein chains (pieces), while B-cell receptors are composed of only 2 pieces.

D. T-cell receptors are eventually secreted into the bloodstream by activated T-cells, whereas B-cell receptors are not; they always stay with the B-cell.

Answer 67

A. T-cell receptors must have antigen broken down inside a cell and presented to them by a Major Histocompatibility Complex (MHC) molecule.

Question 68

Why would a person who has their tonsils removed be more susceptible to certain types of infections of the throat and respiratory tract?

A. Tonsils produce high levels of lactoferrin, a strong natural antibacterial compound.

B. Tonsils produce large amounts of interferons, natural antiviral compounds.

C. Tonsils are secondary lymphoid organs-they help to provide a constant response to the microbes in the oral cavity, helping to keep them in check and preventing them from spreading to other areas.

D. Tonsils are the location where T cells develop and mature. Without them, a person won’t have T cells, and will be more likely to suffer from infections that would normally be eliminated by such cells.

Answer 68

C. Tonsils are secondary lymphoid organs-they help to provide a constant response to the microbes in the oral cavity, helping to keep them in check and preventing them from spreading to other areas.

Question 69

Would a denatured antigen be expected to have the same epitopes as its native (non-denatured) counterpart? Why?

A. Yes-epitopes are just a sequence of amino acids in a row, so they do not change regardless of 3D shape of the protein molecule they lie within.

B. No-ALL epitopes are dependent on being in the proper original 3D conformation in the protein they arise within. Denaturing them would destroy them by destroying that conformation.

C. Yes AND No-SOME epitopes are dependent on 3D conformation (conformational epitopes), while some simply depend on the primary order of amino acids (linear epitopes). So, really, it depends on the particular epitope.

D. Yes-all proteins must be broken down into individual epitopes for presentation to B and T cells on MHC molecules, so each antigen protein MUST be denatured to yield ANY epitopes.

Answer 69

C. Yes AND No-SOME epitopes are dependent on 3D conformation (conformational epitopes), while some simply depend on the primary order of amino acids (linear epitopes). So, really, it depends on the particular epitope.

Question 70

In opsonization with IgG, why would it be important that IgG react with the antigen BEFORE a phagocytic cell recognizes the antibody molecule?

A. If the IgG bound to the phagocyte BEFORE opsonization, it would most likely be ingested by the phagocyte before it could bind to a pathogen (it would be ‘naked,’ so to speak).

B. Binding of IgG by phagocytes would block the antigen binding sites on the IgG molecules, preventing them from binding to the microbes.

C. Binding of IgG by phagocytes changes their conformation-and by changing their protein conformation, their antigen binding sites are changed and they can no longer recognize their specific antigenic epitopes.

D. Binding of antibody by phagocytes results in immediate release of protein-destroying enzymes to the outside of the cell. Since antibodies are proteins, they would be destroyed by these enzymes (and would then be unable to bind to their specific antigenic epitopes).

Answer 70

A. If the IgG bound to the phagocyte BEFORE opsonization, it would most likely be ingested by the phagocyte before it could bind to a pathogen (it would be ‘naked,’ so to speak).

Question 71

A physician is seeking ways to increase the fine-tuning of antibody immune responses that occurs naturally during affinity maturation. The goal is to create ‘super antibodies’ with intensely high affinity for antigens. She decides to use a drug that can be injected into lymph nodes that will be highly mutagenic specifically to B-cells that are undergoing activation. Is this a good idea? Why or why not?

A. Introducing a highly mutagenic drug into our systems to boost immunity? Are you nuts? This is going to cause cancer!

B. It WILL work, and work well. B-cells naturally have a high degree of mutation in their hypervariable region DNA as they undergo activation, and this is what leads to the possibility of affinity maturation. Boosting that activity will dramatically increase the likelihood of that process.

C. It won’t work. Affinity maturation is a random mutation process, followed by selection of B cells with higher affinity for the antigen in question. It doesn’t matter if you increase the NUMBER of mutations-they still need to be screened for affinity to the antigen, and you can only achieve a certain level of affinity. Beyond that, and any mutations in antibody genes are just ‘extra’ changes without any real effect.

D. The delivery method makes this impractical. It might work, but there are many lymph nodes around the body. During an infection, they would ALL be filled with B cells undergoing the process of affinity maturation. How would you deliver the drug to all the lymph nodes in every area of the body?

Answer 71

C. It won’t work. Affinity maturation is a random mutation process, followed by selection of B cells with higher affinity for the antigen in question. It doesn’t matter if you increase the NUMBER of mutations-they still need to be screened for affinity to the antigen, and you can only achieve a certain level of affinity. Beyond that, and any mutations in antibody genes are just ‘extra’ changes without any real effect.

Question 72

Why would a person who has AIDS be more susceptible to the bacterium that causes tuberculosis?

A. HIV (which causes AIDS) directly infects and destroys CD8+ T-cells. These are the cells that would actively destroy the bacterium that causes tuberculosis.

B. HIV (which causes AIDS) directly inhibits the production of interferons. Interferons have a strong natural antibacterial activity, and are necessary for elimination of the bacterium that causes tuberculosis.

C. HIV (which causes AIDS) destroys CD4+ helper T-cells. These are the cells that help activate and increase the bacteria-destroying capabilities of macrophages. Activated macrophages are required to help clear out the bacterium that causes tuberculosis, so without the CD4+ T-cells, we won’t have activated macrophages.

D. HIV (which causes AIDS) directly infects and destroys antibody-producing B-cells. Without the ability to produce antibodies, we can’t opsonize and ingest/destroy the bacterium that causes tuberculosis.

Answer 72

C. HIV (which causes AIDS) destroys CD4+ helper T-cells. These are the cells that help activate and increase the bacteria-destroying capabilities of macrophages. Activated macrophages are required to help clear out the bacterium that causes tuberculosis, so without the CD4+ T-cells, we won’t have activated macrophages.

Question 73

A terrorist mad scientist develops a new blood-borne virus that will completely shut down presentation of viral epitopes on MHC molecules in the cells it infects. He produces an internet video describing it and how it will be indestructible by CD8+ cytotoxic T-cells and will kill millions (if not billions) of people. The medical community quickly denounces and discredits his plan as impossible, and the whole thing is quickly forgotten-why?

A. CD8+ T-cells are not the cells that are responsible for killing virally-infected cells. The terrorist mad scientist is a misinformed idiot.

B. While CD8+ T-cells ARE important for eliminating a viral infection, they are not the ONLY things that are capable of doing so. Natural Killer cells can kill virally-infected cells that have shut down MHC antigen presentation, and interferons can assist in clearing virally-infected cells.

C. A blood-borne virus would not be capable of rapidly infecting millions of people, due to its difficult mode of transmission.

D. B-cells would be primed right away to produce complement proteins to destroy the virus. This would prevent cells from being infected with it in the first place. His plot would be foiled.

E. While CD8+ T-cells ARE important for eliminating a viral infection, they are not the ONLY things that are capable of doing so. Natural Killer cells can kill virally-infected cells that have shut down MHC antigen presentation, and interferons can assist in clearing virally-infected cells AND a blood-borne virus would not be capable of rapidly infecting millions of people, due to its difficult mode of transmission.

Answer 73

E. While CD8+ T-cells ARE important for eliminating a viral infection, they are not the ONLY things that are capable of doing so. Natural Killer cells can kill virally-infected cells that have shut down MHC antigen presentation, and interferons can assist in clearing virally-infected cells AND a blood-borne virus would not be capable of rapidly infecting millions of people, due to its difficult mode of transmission.

Question 74

The best possible analogy available below for the way in which variable (V), diversity (D), and joining (J) antibody gene segments get put together to create the diversity possible in hypervariable regions is

A. to think of the various segments as a deck of cards-when you get dealt a hand of 5 cards, you have a very high likelihood of getting a different hand every time. The quality of the hand you have dealt will dictate whether or not you have a ‘winning’ hand (capable of binding to antigenic epitopes).

B. to think of the various segments as the pieces of a house-you need a strong foundation first (the joining segments), followed by a frame (the diversity segments), then the interior walls (the variable segments) before the structure is complete.

C. to think of the various segments as building a highway-you need to prepare the area first by clearing a path (the joining segments do this), then grade/slope the area (the diversity segments) before you can finally lay down the asphalt (the variable segments).

D. to think of the various segments as a bingo game-each segment is randomly selected, but you’re going to need 1 of each V, D, and J to form a functional molecule. The ‘right’ combination varies depending on which antigen is eventually going to be binding to the molecule (i.e. your bingo card would be the eventual antigen, and the random calling out of the number/letter combinations would be the forming of the VDJ hypervariable region).

Answer 74

D. to think of the various segments as a bingo game-each segment is randomly selected, but you’re going to need 1 of each V, D, and J to form a functional molecule. The ‘right’ combination varies depending on which antigen is eventually going to be binding to the molecule (i.e. your bingo card would be the eventual antigen, and the random calling out of the number/letter combinations would be the forming of the VDJ hypervariable region).