Humoral immunity - B cell diversity

Question 1

What is the structure of an antibody?

Answer 1

• tetrameric protein - 2 identical heavy chains and light chains
• Light chains either kappa or lambda
• Each chain has a variable region - AA sequence differing between Ig molecules
• this region binds Ag (FAB)
• Hypervariable region has complementarity determining regions (CDRs) and framework regions
• Each chain also has a constant region - responsible for effector functions

Question 2

How does clonal expansion start?

Answer 2

• Body generates over 100million different B cells making a different random Ig
• During an infection, a small number of B-cells will by chance be making an Ig that binds to the foreign Ag
• The cell that makes that Ig will be activated and multiply - Clonal expansion
• Most pathogens will have multiple epitopes, so there will be a number of activated B cells - gives polyclonal response

Question 3

What is also required for activation?

Answer 3

• Direct involvement of CD4+ Th cells (Th1)

- Cytokines released by the Th cell

Question 4

How do we generate diversity in the kappa light chain gene?

Answer 4

• Has 1 constant region segment, 35 V segments and 5 short J (joining) segments
• The J segments are close to C, but V segments are far away on the DNA
• There is a binding site for an endonuclease enzyme after each V segment and in front of each J segment - will randomly cut 1 V and 1 J
• The free ends are then ligated together (dsDNA joining) to give a functional protein

Question 5

Briefly what is the process of getting the kappa chain protein from the germline DNA?

Answer 5

• Germline DNA -> DNA rearrangement -> active gene
• There is a promoter in front of each gene, where transcription will start - gives the precursor RNA (in nucleus)
• After splicing, we will have the mRNA in cytoplasm - will have V,D and J region
• mRNA is translated and then secreted

Question 6

How many different variable regions can be generated from kappa light chain?

Answer 6

1C, 35V, 5J -> 175 possibilities

Question 7

What are the events that occur during VDJ recombination?

Answer 7

• Recognition sequences on the DNA that binds recombinase enzyme
• One of the major proteins in the recombinase is RAG1/RAG2
• Binds to the recognition site on the V or J region
• Cut the DNA, discard the loop in the middle and then cap off the ends of the DNA using hairpin loops
• They then open up the ends and reattach them after a bit more processing

Question 8

Why is there even more diversity generated from this junctional variation?

Answer 8

• before the free ends are ligated together, an exonuclease will process the ends
• Terminal deoxynucleotidyl transferase (TdT) randomly adds a few nucleotides
• This causes extra random variation at the site of N nucleotide action
• The V-J join and this further variation at the joins create the most variable region - CDR3

Question 9

What is the importance of TdT?

Answer 9

• For generating Ig and TCR gene diversity
• As a leukaemia marker - In ALL cell is arrested in early development stage, where cells are still making TdT
• Useful enzyme in genetic engineering/ recombinant DNA work

Question 10

Which bits of DNA (gene segments) encode which bit of kappa light chain polypeptide?

Answer 10

• V segment = variable region
• VJ join = CDRIII
• C = constant region

Question 11

How do we make the lambda light chain gene?

Answer 11

• Slightly more complex

- Generates a similar number of possibilities

Question 12

What diversity is generated by rearrangement of gene segments in the heavy chain?

Answer 12

• Same process as the light chain, however now there are also 20 Diversity (D) segments
• Exonuclease and TdT can add further variation at both the V-D and D-J junctions
• So more possibilities as 2 separate junctions

Question 13

Which bits of DNA (gene segments) encode which bits of heavy chain polypeptide?

Answer 13

• V = variable
• VDJ = CDRIII
• C = constant

Question 14

What is allelic exclusion?

Answer 14

• Any B-cell has two alleles of the Ig heavy chain, in theory it could make 2 different heavy chain proteins - never happens due to allelic exclusion
• Once one allele successfully rearranges and starts making heavy chain proteins, the gene rearrangement process for heavy chains turns off - one B cell only makes one heavy chain
• This is the same in light chains
• B-cell has 2 alleles of kappa and 2 alleles of lambda gene
• In theory could make 4 different proteins
• As soon as one allele makes the protein, the rearrangement process turns off
• One clone of B-cell only makes kapp or lambda
• Polyclonal B cells will be a mixture of cells making either kappa or lambda

Question 15

What happens if a patient is only making one kind of chain?

Answer 15

Light chain restriction

Question 16

What happens in rearrangement of TCR genes?

Answer 16

• TCR is Ag receptor

- Works almost the same