3 - DNA Repair And Cancer

Question 1

What can cause mutagenesis?

Answer 1

• *EXOGENOUS SOURCES:**
• Free radicals

• Ionising radiation (food, x-rays, background)
• Anti-cancer drugs
• Mutagenic agents

ENDOGENOUS SOURCES:

- Replication erros

• Transposable elements
• Free radicals

SPONTANEOUSLY

Question 2

Where do free radicals come from?

Answer 2

• Mitochondria
• Smoking
• WBC
• UV
• Radiation

Question 3

Can mutations be repaired?

Answer 3

Yes, by DNA repair mechanisms but sometimes these mechanisms fail so there is a mutation

Question 4

What is DNA replication stress?

Answer 4

Inefficient replication that leads to replication fork slowing, stalling and or breakage. Leads to mutations

• Replication machinery defects
• Fork progression hinderance
• Defects in reponse pathways

Question 5

What is a mosaic karyotype?

Answer 5

47,+21/46,N

Due to non-disjunction occur in first few mitotic divisions

Question 6

Why can replication machinery defects lead to mutations?

Answer 6

• DNA polymerase may incorporate wrong base accidentally
• Exonuclease domain misfunctional so can’t remove it
• Increased mutation rate

Question 7

What factors can slow down fork progression?

Answer 7

• DNA lesions (dimers due to UV)
• Transcription occuring
• Looping
• Repetitive sequences

Question 8

Why do dimers result in mutation?

Answer 8

Have to wait for DNA damage response to occur before replication can continue.

Therefore replication has slowed so DNA replication stress

Question 9

Why do nucleotide repeats lead to mutations?

Answer 9

FORK SLIPPAGE

Backward leads to insertion

Forward leads to deletion

Question 10

What is Huntingtons disease?

Answer 10

• Trinucleotide repeat disorder of CAG
• Normally it is 6-39 repeats
• 35-121 is Huntingtons
• The more repeats you have the earlier the onset
• Autosomal dominant
• Mutant misfolded protein accumulates in neurons so neurodegenerative disease (mainly basal ganglia)

Question 11

What is the function of the normal protein for the HTT (huntingtons) gene?

Answer 11

Unknown

Question 12

What is the mechanism behind HD?

Answer 12

• Backward fork slippage of trinucleotides during DNA replication
• Loops straighten out for second replication so new DNA is three nucleotides longer, continues

Question 13

What is the DNA damage response pathway?

Answer 13

1. Sensor will detect DNA damge
2. Send signal to transducers
3. Sends signals to effectors

Question 14

Why are there cell cycle checkpoints?

Answer 14

Temporary arrest to allow DNA repair

Question 15

What is the issue with a cell that undergoes senescence?

Answer 15

• It enters G0 as it has mutations but can still function
• May pick up more mutations and reenter G1, which could lead to uncontrollable division

Question 16

What are the DNA repair mechanisms?

Answer 16

- DNA polymerase exonuclease (during replication)

- Base-excision repair (single strand and deanimation)

- Nucleotide excision repair (bulky adducts)

- Mismatch repair

- Non-homologous end joining

- Homologous directed repair

Question 17

How is a double strand break fixed?

Answer 17

Non-homologous: (X)

1. Break recognised by proteins
2. KU70/80 protein form ring around ends to protect ends
3. DNA-PKcs trim nucleotides off end
4. DNA ligase fuses strands back together
5. Mutation as loss of nucleotides

Homologous (Y)

1. Exonucleases cut strands to form single strands
2. Single strands complementary to non sister chromatids so invade the double helix from both directions forming holiday junction
3. Non-sister chromatids act as a template and DNA polymerase and ligase work together

Question 18

Why do we have to do HR and NHR if it causes mutations?

Answer 18

• DNA not protected by telomeres otherwise and so they can’t undergo mitosis/meiosis

Question 19

What is intratumour heterogeneity?

Answer 19

Tumour has subclones due to different mutations, mosaicism

Question 20

What can cause carcinogenesis?

Answer 20

• DNA Replication Stress
• If there is a fault in the DNA damage response so cells not killed when mutation

Question 21

What is the multi-step cancer model?

Answer 21

Mutiple mutations have to occur for a cell to become malignant. DNA repair mechanisms can usually prevent it

Question 22

What is the issue with chemotherapy?

Answer 22

1. Can induce mutations as radiation and selection pressure
2. Forms heterogenous tumour (chemo may kill one subclone but allow survival of the fittest of another)

Question 23

What are synthetic lethality strategies?

Answer 23

• Normal cells may have two genes that aid cell survival
• Cancer cell may have one of those genes not working, e.g gene A
• Produce a drug that targets gene B so cancer cells die as they have no gene A but normal cells survive as they have gene B for back up

Question 24

What is an example of a synthetic lethality strategy?

Answer 24

PARP inhibitor for breast cancer treatment

• Breast cancer cells not good at repairing double strand break but normal cells can
• Inhibiting PARP causes lots of DSB’s
• Cancer can’t fix these so apoptosis but normal human cells can

Question 25

What is xeroderma pigmentosa?

Answer 25

Autosomal recessive disorder where you have a decreased ability to repair DNA damage, e.g damage done by UV light

Question 26

What cells are in G0 for life?

Answer 26

• Neurones
• RBC
• Skeletal muscle
• Retinal cells

Question 27

What do telomeres do and what does telomerase do?

Answer 27

Telomeres: Protect chromosomes from damage and prevent chromosomes fusing together

Telomerase: A reverse transcriptase that prevents telomeres shortnening when primers are formed on telomeres