Humoral immune response

Question 1

Humoral immune response

Answer 1

Part of the adaptive response
Mediated by B cells (B cells differentiate into plasma cells and produce Ab)

Antibodies are the effectors

Goal is to neutralize and eliminate extracellular antigens

If Ag inside of cell, Ab cannot get to it

Question 2

B cell response to antigens

Answer 2

B cell recognizes microbe/Ab

Helper T cells, other stimuli facilitate activation of B cells

Proliferation

Differentiation to:

• to antibody secreting plasma cells = antibody secretion
• always happens*
• IgG-expressing B cell = Isotype swtiching
• high-affinity Ig-espressing B cell = memory B cell or Affinity maturation
• Other steps depend if T cell involved or not *

Antigens and other signals can:

• stimulate proliferation and differentiation of B cels
• IgM synthesis and secretion (small amount)
• Enhance B cell ability to interact with Th cells (responsiveness, migration)

Multivalent antigens vs proteins
-induce different responses

Question 3

B cell response to antigens: protein antigens

Answer 3

Th cells help B cells respond protein antigens
T cells can only recognize peptides derived from proteins when presented on MHC molecule
induce a T-dependent B cell activation

Question 4

B cell response to antigens: multivalent antigens

Answer 4

Polysaccharides, nucleic acids, lipids
Contain the same structural unit repeated multiple times in tandem
Stimulate antibody production without the involvement of Th cells (T-independent activation of B cells)
Can recognize without any type of presentation

Question 5

B cell response to antigens: T dependent

Answer 5

Follicular B-cells (B2 cells)

Question 6

B cell response to antigens: T independent

Answer 6

Marginal zone B cells and B1 cells

Innate like B cells: broad specificity BCRs and TLR

Question 7

T dependent

Answer 7

Protein antigen onto follicular B cells
Helper T cells attach
Isotype switched, high affinity antibodies; memory B cells, long lived plasma cells

Question 8

T independent

Answer 8

Polysaccharide antigen onto B-1 cells, marginal zone B cells (multivalent, allows cross linkage of B cell receptors)
Other signals (like complement protein, microbial product)
Mainly IgM, low-affinity antibodies; short-lived plasma cells

Question 9

Germinal center formation

Answer 9

A. Independent activation of T and B cells
Interaction at the edge of follicles
T cells need to be primed by DCs first
B cells can recognize Ag on own

B. Initial plasma cell activation
Migration of B and T cells to follicle (B cell zone)
Germinal center formation

Question 10

Germinal centers

Answer 10

Sites where B cells grow undergo maturation
Ag specific B cell activated and stimulated and starting proliferation will produce germinal centers
Round-ovoid clusters of cells
Divided into light and dark zones
Originates from antigen-specific B cells

Places where you will have proliferation afterAg stimulation
“where the magic happens”

Activation of B cells and migration into germinal center
B cell proliferation
Somatic mutation and affinity maturation; isotype switching
Exit of high-affinity antibody secreting cells and memory B cells

Question 11

Th cells co-stimulation

Answer 11

In primary response: DC presenting Ag to Tcell

In secondary response: already activated T cells
IL-1 interacts with Th cells

T and B cell interaction

Question 12

CD40/CD40L (CD154) co-stimulation

Answer 12

CD154 (Th cell) ->

• B cell (CD40) : proliferation; Ig production; Ig class switching
• Dendritic cell (CD40): antigen presentation; cytokine production; cell survival
• Macrophage (CD40): cytokine production; activation

Question 13

Th cell co-stimulation

Answer 13

Activated helper T cell expresses CD40L, secretes cytokines
B cells are activated by CD40 engagement cytokines
B cell proloferation and differentiation

Question 14

CD40/CD154L co-stimulation

Answer 14

CD40-CD154 (CD40L) up-regulates expression of IL-4 and IL-4 receptors on B cells
Signals from CD40 synergize with IL-4 and IL-5 receptors
B cell activation, memory cell development and Ig class switching
(IL-4 usually secreted by Th2)

Question 15

Cytokine secretion by Th2 cells: IL-4

Answer 15

Wont have in T-independent
growth and differentiation of B cells
Increased expression of MHC II
Induces Ig class switching

Question 16

Cytokine secretion by Th2 cells: IL-5

Answer 16

B cell -> plasma cells
Increased IgM and IgG production
IL-5 and IL-4 increase IgE production
Selectively increase IgA production

Question 17

Cytokine secretion by Th2 cells: IL-6

Answer 17

Needed for final differentiation of B cell into plasma cells
IL-6 and IL-5 increase IgA production
IL-6 and IL-1 increase IgM production

Question 18

Cytokine secretion by Th2 cells: IL-13

Answer 18

similar to IL-4

Required for optimal production of IgE

Question 19

Innate co-stimulation

Answer 19

A. C3d bound to microbes
Simultaneous binding of: C3d-CR2 (CD21)
Microbial antigens-BCR

B. PAMPs
Simultaneous binding of: PAMP-TLR
Microbial antigens-BCR

Question 20

Plasma cells

Answer 20

Develop from antigen stimulated B cells
Spleen, the medulla of lymph nodes, and the bone marrow
10,000 Ig/second
V active metabolically

At least two population:
- (t ind) short-lived population: 1-2 weeks and produces large amounts of antibodies after antigen exposure

-(tdep) long-lived population: months or years and accumulate in the bone marrow (if exposed a 2nd time, have enough Ab to block it w/o becoming sick)

Question 21

Memory cells

Answer 21

2 populations:
-Long lives resting cells (IgG BCR). Survival do not depend on antigen contact
(if encounter Ag quickly activate and facilitate secondary response)

-large and dividing memory cells (IgM BCR). Survival depends on antigen contact

Survival in humans up to 60 years

Question 22

Primary vs secondary Ab response

Answer 22

Enough Ag for first time encounter naive B cell. Becomes activated and proliferates. Predominance of IgM in 1st response

Much easier to activate in second response because of memory cells
The magnitude of second response is greater
More IgG produced second time

Question 23

Primary Ab response

Answer 23

Lag after immunization: usually 5-10 days
Peak response: smaller
Ab isotype: usually IgM > IgG
Ab affinity: Lower average affinity, more variable

Question 24

Secondary Ab response

Answer 24

Lag after immunization: usually 1-3 days
Peak response: larger
Ab isotype: Relative increase in IgG and under certain situations in IgA or IgE (heavy chain isotype switching)
Ab affinity: higher average affinity (affinity maturation)

Question 25

B cell receptors

Answer 25

200,000 to 500,000 BCRs in each cell
Antigen binding and signaling components
Immunoglobulin superfamily

Question 26

Immunoglobulin structure

Answer 26

4 polypeptide chains

• two identical heavy chains
• two identical light chains
• constant and variable regions in each chain

Fab- fragment antigen binding
Fc- fragment crystallizable

Reduce and acidify: isolated chains
Papain: papain fragments (Fab, Fc)
Pepsin: Pepsin fragments (F(ab’)2, pFc’)

Hinge regions: allows arms to move around and adjust

Question 27

Heavy chains

Answer 27

400-500 amino acids divided in 4-5 domains
1 variable domain (Vh)
3-4 contant domains (Ch)
five types of HC:
-a, y, d, e, u
-differences in aa sequence, domain structure and biological activity
-determines the Ig class

Question 28

Light chains

Answer 28

220 amino acids in 2 domains
1 variable domain (Vl)
1 constant domain (Cl)
Two types of LC:
-k, l
-functionally identical (can change light chain without changing any function overall

Question 29

Antigen binding site

Answer 29

Composed by the variable domains in light and heavy chains
(is the cleft between the chains)
-framework regions: hold complimentary regions together kind of and offer stability, allows molecules to remain in same general structure
-Complementary determining regions (hypervariable): may mutations- vary a lot in structure and conformation

Question 30

CDRs

Answer 30

Sequence variation in 6 to 10 amino acids in three regions of the variable domain 
Constant regions (framework regions) in between CDR

Will change how attach and fit with epitope : lock and key

Question 31

BCR’s signal transducing component

Answer 31

The BCR itself cannot signal directly to the cell

Associates with glycoprotein heterodimers formed by pairing CD79a (Ig-a) with CD79b (Ig-B)

Question 32

Antibodies

Answer 32

Soluble BCRs
Divided in 5 classes (type of HC)
-IgG- y HC
-IgM- u HC
-IgA- a HC
-IgE- e HC
-IgD- d HC

Question 33

IgG

Answer 33

Y heavy chain- 4 domains
180 kDa MW
Very mobile (hinge region)
Small size = can move to tissues
The most abundant in serum

Question 34

IgG functions

Answer 34

Most versatile
Neutralization of microbes nad toxins
Opsonization of antigens
Activation of the classical pathway of complement
Antibody dependent cellular cytotoxicity (NK cells) (ADCC)
Neonatal immunity

Question 35

IgM

Answer 35

u Heavy chain-5 domains in each subunit
5-6 subunits per molecule
900 kDa MW (polymeric form)
No hinge region

Question 36

IgM functions

Answer 36

Second highest concentration in serum
Major Ig of the primary immune response
More efficient than IgG at complement activation
Rarely enter tissue fluids (bc of size)

Question 37

IgA

Answer 37

a heavy chain- 4 domains in each subunit
2-3 subunits per molecule
Usually secreted as a dimer (360 kDa)
Produced in body surfaces and transported through epithelial cells into external secretions

Question 38

IgA functions

Answer 38

Does not activate the classical complement pathway
Mucosal immunity
Neutralization of microbes and toxins
Located in different part of the body too

Secreted by mucosal plasma cells
Binds to receptors (pIgR) on the interior intestinal enterocytes
Passed in vesicles to the cell surface
In the intestinal lumen, the pIgR is cleaves
Secretory component

Question 39

IgE

Answer 39

e Heavy chain- 5 domains
presents a hinge region
190 kDa molecular weight
Low concentrations in serum

Question 40

IgE functions

Answer 40

IgE triggers the release of inflammatory molecules from the mast cells
Mediates type I hypersensitivity reactions (allergic rxns)
Responsible in part for immunity to parasitic worms
Shortest half-life of all immunoglobulins (2-3 days)

Question 41

IgD

Answer 41

d Heavy chain- 4 domains
Presents a hinge region
170 kDa MW
IgD is mainly found attached to B cells
Bonds between HC not strong so degrades easily

Question 42

IgD functions

Answer 42

Found in horses, cattle, sheep, pigs, dogs, rodents, and primates
Not detected in rabbits or cats
Does not have a clear role
In humans, IgD binds to basophils -> IL-4, IL-1, cathelicidins, and B cell activator factor

Question 43

Isotype distribution within the organism: IgA

Answer 43

Neutralize things that invade body so it is in secretions and mucosal tissues
Respiratory tract, gut mucosa, mouth etc

Question 44

Isotype distribution within the organism: IgE

Answer 44

Epithelial, subQ, and some mucosal tissues

Mast cells

Question 45

Isotype distribution within the organism: IgG

Answer 45

Smallest and can diffuse through tissues- most versatile so it like everywhere

Question 46

Isotype distribution within the organism: IgM and IgG

Answer 46

in blood

IgM is too big to leave easily

Question 47

Immunoglobulin varients

Answer 47

Isotype
Allotype
Idiotype

Question 48

Isotypes

Answer 48

Classes and subclasses (shared via species)- more than one type of IgA or IgG etc
Result of gene duplication

Question 49

Allotypes

Answer 49

Variations in immunoglobulin amino acid sequences (not associated with Ag specificity)
Ig of one individual may differ from those of another individual of the same species
(minor differences)

Question 50

Idiotypes

Answer 50

Variations in the amino acid sequences within the variable domains on light and heavy chains
(like for all the different illnesses they have come accross)
Each individual with have a large number of different idiotypes

Question 51

Class switching

Answer 51

Switch from IgM production to IgA production by deleting intervening heavy chain genes and joining the V genes to the appropriate heavy chain gene

Change the isotype without altering its Ag specificity
Dont change variable domain- bc dont want to change affinity for the Ag- kind of rearrange stuff

Question 52

Antigen-antibody binding

Answer 52

Interaction between chemical groups on the surface of the antigen and on the CDRs
Non-covalent bonds (need enough to generate a stable binding bc they are weak bonds)
Requires a close conformational fit (lock and key)

Question 53

Affinity

Answer 53

Refers to the strength of binding of one Fab of an antibody to one antigenic epitope
The sum of attractive and repulsive forces between the epitope antigen-binding

Question 54

Avidity

Answer 54

Refers to the strength of overall binding of the two molecules
Increasing affinity can increase avidity

Question 55

Affinity maturation

Answer 55

Antigen concentration declines after the start of the Ab response
-only successively higher affinity cells will bind sufficient antigen to maintain proliferation ( need to be encountering Ag)

High rate of mutation in the germinal centers
-mutants with an advantageous higher affinity will bind well with antigen -> positive selection for persistent clonal expansion

B cell activation by protein antigen and helper T cells
B cells with somatically mutated Ig V genes and Igs with varying affinities for antigen
B cells with high affinity membrane Ig bind antigen on follicular dendritic cells (FDCs) and present antigen to helper T cells
B cells that recognize antigen on FDCs or interact with helper T cells are selected to survive; other B cells die

Question 56

Antibodies as effectors

Answer 56

Neutralization of microbes and toxins
Opsonization and phagocytosis of microbes
Antibody dependent cellular cytotoxicity
Lysis of microbes
Phagocytosis of microbes opsonized with complement fragments
Inflammation
Complement activation

Question 57

Antibodies as effectors IgG

Answer 57

Neutralization of microbes and toxins
Opsonization of antigens for phagocytosis by macrophages and neutrophils
Activation of the classical pathway of complement
Antibody-dependent cellular cytotoxicity mediated by NK cells
Neonatal immunity: transfer of maternal antibody across placenta and gut
Feedback inhibition of B cell activation

Question 58

Antibodies as effectors IgM

Answer 58

Activation of classical pathway of complement

Question 59

Antibodies as effectors IgA

Answer 59

Mucosal immunity: secretion of IgA into lumens of GI and respiratory tracts, neutralization of microbes and toxins

Question 60

Antibodies as effectors IgE

Answer 60

Eosinophil and mast cell medicated defense against helminths

Question 61

Neutralization of microbes and toxins

Answer 61

A. Without antibody: microbe entry through epithelial barrier
With antibody: antibody blocks penetration of microbe through epithelial barrier

B. without antibody: infection of cell by microbes
With antibody: antibody blocks binding of microbe and infection of cells

C. Without antibody: Pathologic effect of toxin
With antibody: antibody blocks binding of toxin to cellular receptor

Question 62

Receptors for antibodies

Answer 62

Fcy means that its a receptor for IgG, Fce means IgE.

FcyRI has a high affinity for Ig

Question 63

Receptors for antibodies: FcyRI

Answer 63

High affinity for Ig.
Cell distribution: macrophages, neutrophils, eosinophils
Function: phagocytosis; activation of phagocytes

Question 64

Receptors for antibodies: FcyRIIA

Answer 64

Low affinity for Ig
Cell distribution: Macrophages, neutrophils; eosinophils, platelets
Function: phagocytosis; cell activation (inefficient)

Question 65

Receptors for antibodies: FcyRIIB

Answer 65

Low affinity for Ig
Cell distribution: B lymphocytes, DCs, mast cells, neutrophils, macrophages
Function: Feedback inhibition of B cells, attenuation of inflammation

Question 66

Receptors for antibodies: FcyRIIIA

Answer 66

low affinity for Ig
Cell distribution: Nk cells
Function: Antibody dependent cellular cytotoxicity

Question 67

Receptors for antibodies: FceRI

Answer 67

high affinity for Ig; binds monomeric IgE
Cell distribution: Mast cells, basophils, eosinophils
Function: activation (degranulation) of mast cells and basophils

Question 68

Antibody mediated opsonization and phagocytosis of microbes

Answer 68

Phagocyte cell with Fcy recognizes IgG antibody. signals to phagocitize while thing- opsonization

Opsonization of microbe by IgG
Binding of opsonized microbes to phagocyte Fc receptors (FcyRI)
Fc receptor signals activate phagocyte 
Phagocytosis of microbe
Killing of ingested microbe

Question 69

Antigen-dependent cellular cytotoxicity (ADCC)

Answer 69

Antibody-coated cell with surface antigen
The surface antigen recognizes IgG
Receptor recognizing Fc portion of Ab attached to Ag.
Nk cell to Fc portion of IgG
leads to killing of antibody coated cell

Question 70

IgE

Answer 70

and eosinophil-mediated killing of helminths

Th2 cell releases IL-5 which acts on eosinophil
FceRI on the eosinophil recognize FC regions of IgE
binds helminth
Eosinophil activation
Helminth death