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Question 1

Antibodies are the effector molecules (globular proteins) produced in LARGE (not small) quantities by __ cells

Answer 1

B. Specifically plasma cells.each antibody produced by a single B cell has the exact same specificity for antigen

Question 2

What do antibodies do?

Answer 2

they simply bind to specific ligands on the surface of pathogens. These PROTEINS have no toxic properties and do not themselves destroy invading pathogens. Because antibodies also serve as ligands for receptors on phagocytic cells, when they bind to a pathogen they promote uptake and destruction of the pathogen by phagocytes (opsonization)

Question 3

Additional roles of antibodies.

Answer 3

In addition, some isotypes of antibodies serve as ligands for the 1st component of the classical complement cascade (opsonization). Finally, in some cases binding of antibodies to a pathogen (or pathogen-derived toxin) prevents binding of the pathogen (or toxin) to its host ligand, thereby preventing infection or toxicity (neutralization).

Question 4

Describe the structure of antibodies.

Answer 4

All antibody molecules have a common core structure that consists of two identical “light chains” (approx. 24kD), and two identical “heavy chains” (approx. 55 or 70kD). One of the two light chains is attached to each heavy chain, and the heavy chains are attached to each other; these attachments are formed by intrachain disulfide bonds.

Question 5

T or F. heavy and light chains are encoded on the same genesWhat are lg domains?

Answer 5

F. They are encoded on separate genesheavy and light chains consist of a series of similar (not identical) sequences (domains); about 110 residues in length (Ig domains)immunoglobulin (Ig) domains fold independently, interchain disulfide bonds help form the domainsthe amino-terminal Ig domain of each chain (variable region) is highly variable between different Abs; the remaining domains are conserved (constant regions)

Question 6

Note on domain structure.

Answer 6

the constant (C) domains and variable (V) domains of all antibody molecules have a similar structure; it is important toremember that Abs perform their functions in extracellular spaces in the presence of infection, where they encounter variations in pH, salt concentration, proteolytic enzymes, and other potential destabilizing factors; their unique tertiary structure enables them to withstand these environmental factors and maintain their functionality

Question 7

Describe the shape of the C and V domains of antibodies.

Answer 7

both C and V domains are a roughly cylindrical shape and are formed by two adjacent β-sheet structures that are covalently linked by an intrachain disulfide bond

Question 8

the adjacent β-sheets of C and V domains form structures known as a _____.

Answer 8

a β-barrel or β-sandwich (a β-barrel is a common secondary structural motif of proteins)

Question 9

B-barrels formed in antibody molecules are called?

Answer 9

immunoglobulin folds

Question 10

What is the primary difference between C and V domains?

Answer 10

V domains are larger and have extra loops of polypeptide chain

Question 11

The extra loops of polypeptide chain in the V domains form what?

Answer 11

the flexible loops of V domains form the antigen-binding domainsABDs are found in located regions on BOTH the heavy and light chains

Question 12

A variability plot in which the amino acid sequences of the V domains of many heavy and light chains have been compared, revealed that sequence variability in confined to 3 distinct regions within these variable domains. What are they?

Answer 12

1. hypervariable regions (HV) are designated HV1, HV2, and HV3 (or complementarity-determining regions CDR1-3).2. the low variability regions between these hypervariable regions are known as framework regions (FR1, FR2, FR3, and FR4)

Question 13

What do the framework regions of the V domains (FR1-FR4) form? What about the hyper variable (HV) sequences

Answer 13

the B-sheets that provide the structural framework of the domains, while the hypervariable sequences correspond to the loops between the β-sheetstherefore, the hypervariable regions are localized to a particular surface of the immunoglobulin molecule

Question 14

How do the HV regions of the light and heavy chains in an antibody interact?

Answer 14

when the heavy chains and the light chains are paired in an antibody molecule, their hypervariable regions are brought together, creating a single hypervariable site at the tip of each “arm” of the antibody molecule. This conjoined hyper variable site forms the antigen-binding site

Question 15

The antigen binding regions of an antibody molecule are aka?

Answer 15

the idotype of the antibody

Question 16

What is idiotype?

Answer 16

term to describe the 3D or tertiary structure of the antigen binding site of an antibody. The idiotype is essentially the shape of the antigen-binding site that accommodates the shape of a particular antigen

Question 17

T or F. Each antibody molecule has only a single idiotype. Why or why not?

Answer 17

T. because both of the antigen-binding sites of any antibody monomer are identical, and therefore, they have an identical shape.

Question 18

The region of the antigen on an invading micro-organism that is recognized by the antibody by its HV regions is called?

Answer 18

an antigenic determinant or EPITOPE

Question 19

Again, what is the function of antibodies?

Answer 19

the function of antibodies is to bind to microorganisms and to facilitate their destruction and removal from the body

Question 20

Antibodies produced during INFECTION usually have specificity for what kinds of epitopes?

Answer 20

those that are composed of eithercarbohydrate or protein (remember, the surface of pathogens typically are composed of glycoproteins, polysaccharides, glycolipids, and proteoglycans)

Question 21

What are multivalent antigens?

Answer 21

Antibodies typically have specificity for epitopes that are composed of carbs or proteins. Complex macromolecules like these typically have multiple epitopes, each of which can be bound by a separate antibody molecule (but those antibodies don’t necessarily have to be distinct)

Question 22

T or F. a multivalent antigen can have a single epitope that is repeated many times, or it can have a number of distinct epitopes

Answer 22

T. Repeat: a multivalent antigen can have a single epitope that is repeated many times, or it can have a number of distinct epitopes. What is the significance of this?Most pathogens are multivalent

Question 23

Can antibodies be produced that have specificity for epitopes that care composed of things other than carbs or proteins? If so, what are they typically used for?

Answer 23

Yes. Such antibodies are involved in allergic reactions and autoimmune diseases and are not involved in defense against infection (e.g. antibodies specific for DNA are characteristic of systemic lupus erythematosus)

Question 24

The binding of ABs to antigens (via what regions on each?) is based solely on what kinds of forces?

Answer 24

non-covalent forces (electrostatic forces, hydrogen-bonding, van der Waals forces, and hydrophobic interactions)

Question 25

How are van der Waals and hydrophobic interactions between ABs and antigens produced? In other words, what characteristic of ABs allows for this to occur?

Answer 25

the antigen-binding regions of antibody molecules are typically rich in aromatic amino acids which can participate in many van der Waals and hydrophobic interactions

Question 26

How do the HV regions of light and heavy chains come together? What do they form to facilitate antigen binding?

Answer 26

the hyper variable regions (orcomplementarity-determining regions or CDRs) of the variable Ig domain of the light and heavy chains come together to form a unique shape that, together with the amino acid side chains that reside in these regions, allows the antibody to bind to a specific epitope; The HV regions of the heavy and light chain come together to form pockets, grooves, or extended surfaces that allow them to bind to their specific antigen.

Question 27

T or F. it is possible that there could be several structurally distinct antibodies that could bind to the exact same epitope

Answer 27

T; however, each of these antibodies could bind to the epitope with different binding strengths

Question 28

The binding strength of any antibody to its particular antigenic determinant is known as?

Answer 28

the binding affinity. NOTE: it is important for you to remember that all non-covalent protein:protein interactions are reversible; an antibody that has high affinity for an antigen stays bound longer than an antibody that has low affinity

Question 29

What is avidity?

Answer 29

the combined binding strength of all antigen-binding domains of an antibody bound to the antibody’s cognate antigen simultaneouslyWhen an antibody is bound to a multivalent antigen via each of its antigen-binding regions, for the antibody to release from the antigen, both of the binding regions would have to release at the same time. Because antibodies typically bind with high affinity to their antigen, the binding equilibrium for each antigen- binding region of the antibody for antigen is shifted strongly to the bound state for both of the antigen-binding regions. The higher the affinity, the less likely that both binding regions will release at the same time.Since IgM has 10 antigen-binding regions (because it is a pentameric), it has the highest potential avidity of any of the antibody isotypes (by far).

Question 30

Antibodies can bind to what two types of antigenic determinants of proteins?

Answer 30

1. continuous epitopes (linear)2. discontinuous epitopes (non-linear)

Question 31

What are continuous epitopes?

Answer 31

a linear or continuous epitope is formed by a linear stretch of amino acids

Question 32

What are discontinuous epitopes?

Answer 32

a non-linear or discontinuous epitope is formed by portions of an antigen that arebrought together due to the arrangement of the antigen; for example: amino acids from different parts of a polypeptide that are brought together when the protein is in its native form (its normal tertiary structure); if that tertiary structure is disrupted, the epitope no longer exists because the antibody contact points are no longer together in a discreet formation

Question 33

antibody molecules can be subdivided into five different isotypes based on the type of heavy chain that is found in the antibody. What are they?

Answer 33

IgA: alpha (α), IgD: delta (δ), IgE: epsilon (ε), IgG: gamma (γ), and IgM: mu (μ).

Question 34

T or F. light chains have a single variable region and a single constant region

Answer 34

T

Question 35

How many V and C regions do heavy chains have?

Answer 35

heavy chains have one variable (V) region and either three (IgG, IgD, and IgA) or four (IgM and IgE) constant (C) regions

Question 36

Which antibodies types have heavy chains with 3 constant regions? 4 constant regions?

Answer 36

3- A, D, G4- E, M

Question 37

What is a hinge region?

Answer 37

rich in proline residues, the hinge region allows flexibility of the Ab molecule that enables it to more easily bind to antigenic determinantsand/or immune components (FcR). These are found only in ABs IgA, D, and G.NOTE: the hinge region of IgG and IgA is sensitive to proteolytic cleavage

Question 38

What are the two types of light chains?

Answer 38

kappa and lamdathese different light chains types can be present in any of the five AB types, BUT only one of these types is found in an individual Ab molecules because each antibody molecule is composed of 2 identical light chains (and two identical heavy chains)

Question 39

What kinds of light chains are IgG Abs composed?

Answer 39

In humans, approx. 60% contain kappa light chains, while 40% contain lama light chains

Question 40

What are the subtypes of IgA Abs?

Answer 40

IgA1 and IgA2

Question 41

What are the subtypes of IgG Abs?

Answer 41

IgG1, IgG2, IgG3, and IgG4. These differ in the structure of the hinge

Question 42

Which Ab isotopes can exist as multimeric structures of Ab molecules?

Answer 42

IgM and IgA

Question 43

What facilitates IgM and IgA Abs being able to exist as multimers (IgM typically as pentameric and IgA typically as dimeric)?

Answer 43

the joining or J chain

Question 44

What is the J chain?

Answer 44

The J chain is a 15 kD polypeptide thatis disulfide linked to the tail-pieces (extensions at the carboxyterminal region of the alpha and mu heavy chains). It functions to stabilize IgA and IgM multimers

Question 45

What are secretory components? Where are they produced?

Answer 45

In mucosal secretions, another polypeptide called the secretory component is attached to the IgA dimer non-covalently. The secretory component of IgA is produced by epithelial cells that line the luminal surface of mucosal tissues. Secretory component on the surface of the cells combines with IgA produced locally by lymphocytes and transports the IgA through epithelial cells (lining mucosal surfaces) into secretions

Question 46

IgA composes what percent of serum immunoglobulin?What is its half-life?

Answer 46

5-15%6 dayscan occur are monodic, dimeric, or trimeric structures (multimerized by J chains)

Question 47

Where can the dimeric form of IgA by found in the body?

Answer 47

colostrum/breast milk, intestinal and respiratory secretions, saliva, tears, and othersecretions

Question 48

IgA-deficient individuals experience increased incidence of what?

Answer 48

respiratory and some gastrointestinal infections

Question 49

IgD composes what percent of serum immunoglobulin?

Answer 49

less than 1%. Not secreted in appreciable amounts and has no known effector role in a humoral immune response

Question 50

What is the primary role of IgD?

Answer 50

exists primarily as membrane IgD; serves with IgM as an antigen receptor on early B cell membranes to help initiate Abresponses by activating B cell growth

Question 51

IgD composes what percent of serum immunoglobulin?

Answer 51

less than 1%.

Question 52

Where is most IgE found?

Answer 52

most IgE is bound to Fc receptors on mast cells where it serves as a receptor for allergens and parasite antigens; if sufficientAg binds to IgE on mast cells, the mast cells degranulate, releasing histamine, prostaglandins, platelet-activating factor, andcytokines

Question 53

IgE is important for protection against ____ and is responsible for ____

Answer 53

parasitic infectionanaphylactic hypersensitivity

Question 54

IgG composes what percent of serum immunoglobulin?half-life?

Answer 54

85% in adults23 days (longest of any isotype)

Question 55

What are the roles of IgG?

Answer 55

• fixes complement (requires multiple IgG molecules)• stimulates chemotaxis• acts as an opsonin, therefore, facilitates phagocytosis• principle antibody isotype in anemnestic (memory) immune responses • crosses the placental barrier

Question 56

IgM composes what percent of serum immunoglobulin?How does it exist?

Answer 56

• comprises 5-10% of total Ig in adults• is secreted as a pentameric molecule (10 heavy chains and 10 light chains) stabilized by a J chain (has 10 antigen-binding domains)

Question 57

Notes about IgM.

Answer 57

is the most efficient Ig for fixing (binding to) complement; a single pentamer can activate the classical complement pathway;promotes phagocytosis and bacteriolysis through complement fixing activity

Question 58

Where is monomeric IgM found?

Answer 58

monomeric IgM is found (along with IgD) on the surface of all naïve B cells; serves as a receptor for antigen

Question 59

Can IgM cross into tissue? Why?

Answer 59

cannot cross efficiently into tissue because of large size

Question 60

IgM are particularly important for immunity to what kinds of antigens?

Answer 60

particularly important for immunity to polysaccharide antigens (cell wall components of bacterial pathogens; T-independentantigens)

Question 61

Each monomeric Ab has how many antigen-combining sites/variable regions (the regions of the Ab which interact with the epitope of the antigen)?

Answer 61

2

Question 62

The stem portion of an antibody is termed the ___ of an Ab?

Answer 62

Fc portion

Question 63

What is the Fc region of an antibody?

Answer 63

the Fc region interacts with complement components and with macrophages and NK cells to promote clearance of antigen and activation of subsequent immune responses.

Question 64

The hinge region of which Abs are susceptible to proteolytic cleavage?

Answer 64

IgG and IgA

Question 65

What does papain do?

Answer 65

enzyme through which cleavage of an IgG or IgA yields a single Fc fragment and two Fab fragments. Each Fab fragment contains a single antigen-binding site

Question 66

The Fc portion of IgG1 and IgG3 Ab are recognized by Fc receptors on what kinds of cells?

Answer 66

macrophages and neutrophils. these cells can therefore bind to and engulf opsonized pathogens

Question 67

The Fc portion of IgE binds to Fc receptors on what kinds of effector cells?

Answer 67

mast cells, basophils, and activated eosinophils. This enables these cells to respond by releasing inflammatory mediators

Question 68

the Fc portions of antibody:antigen complexes can bind to complement, initiating the complement cascade (IgG1, IgG2, IgG3, and IgM)

Answer 68

the Fc portions of antibody:antigen complexes can bind to complement, initiating the complement cascade (IgG1, IgG2, IgG3, and IgM)

Question 69

The Fc portion can facilitate delivery of antibody to sites they would not reach without active transport. Name some examples.

Answer 69

these sites include mucous, tears, and milk (IgA) and fetal blood circulation (IgG1, IgG2, and IgG3)

Question 70

What is the Clonal hypothesis?

Answer 70

During development, progenitor cells give rise to a large number of lymphocytes, each with a unique specificity. During infection, lymphocytes with receptors that recognize pathogens are activated B cells that make pathogen-specific antibodies can clonally expand and produce pathogen-specific antibodies that can mediate clearance of the infection

Question 71

When are plasma cells made?

Answer 71

A resting B cell (made in bone marrow) with a specific membrane bound Ig will recognize a pathogen initially. The stimulated B cell will then give rise to plasma cells which produce free floating/secreted antibodies

Question 72

What is Isotope switching?

Answer 72

B cells can be signaled to produce antibody of a different isotype. Only the constant region of the heavy chain is altered. Differences in the constant chains of Ab isotypes allows maximum versatility of antibody-mediated immune responses