Genomic Instability

Question 1

What does cancer generation require?

Answer 1

Mutation

Question 2

What is genomic instability?

Answer 2

The increased acquisition of genomic alterations

Question 3

What leads to genomic instability?

Answer 3

Defects in mechanisms to protect genomes

Question 4

What are the two general types of DNA damage?

Answer 4

Exogenous and Endogenous

Question 5

List some examples of exogenous damage

Answer 5

UV, x-rays, chemical

Question 6

List some examples of endogenous damage

Answer 6

Metabolism, replication errors, fork stalling

Question 7

How can the byproducts of metabolism result in oxidative DNA damage?

Answer 7

Byproducts include reactive oxygen species with unpaired electron (eg peroxide, hydroxyl radical, superoxide anion) can cause altered bases and strand breaks etc as they can alter chemical composition of DNA

Question 8

State the 2 ways DNA is protected

Answer 8

It’s structure and detoxification

Question 9

How is DNA protected by its structure?

Answer 9

Housed in nucleus so is protected from physical/ chemical damage
Tightly packed, wrapped around his tones, folded into fibres > coils > chromosomes which reduces damage

Question 10

How is DNA protected by detoxification?

Answer 10

Harmful agents are neutralised. Eg:

• via redox pathway
• cell membrane pumps which pump our harmful agents
• enzymes which catalyse harmful agents into safe products
• proteins which conjugate harmful chemicals before they come into contact with cell

Question 11

How does the redox pathway help protect DNA?

Answer 11

Superoxide radical (O2-) is converted to H2O2 by the action of a super-oxide dismutase. 
This can be converted to a damaging hydroxyl radical which damages DNA, but is instead converted to H2O and O2 by catalase or into 2H2O via glutathione peroxide, both of which are not harmful to DNA

Question 12

List the classes/types of DNA damage

Answer 12

• loss of base
• small additions to nucleotides (adducts)
• bulkier adducts
• single or double strand breaks
• mismatched bases
• cross links in DNA within and between strands

Question 13

Describe the most common example of small adduct DNA damage

Answer 13

Most common in 8oxo-G where oxygen is added to the 8th carbon of guanine under oxidative stress. Changes structure of guanine

Question 14

What happens if small adducts go unrepaired?

Answer 14

Base pairs in corrects, eg 8-oxoG to A instead of C

Causes mismatch during replication

Question 15

Describe bulky adducts and give an example

Answer 15

Big changes in structure
Eg: benzopyrene (polycyclic aromatic hydrocarbon) present in polluted air, food, cigarette smoke, is a big adduct onto guanine

Question 16

What happens if a bulky adduct goes unrepaired?

Answer 16

Can distort DNA helix which blocks replication and stalls transcription

Question 17

Describe single strand breaks

Answer 17

Loss of a single nucleotide, 5’ and 3’ termini damaged at end of breaks

Question 18

What happens if a single strand DNA break goes unrepaired?

Answer 18

Can block DNA replication and stall transcription

Question 19

What is the difference between double strand and single strand breaks?

Answer 19

Double strand loses bases in both strands so there is so template to copy lost info from unlike single strand breaks.

Question 20

What happens if double stranded breaks go unrepaired?

Answer 20

Risk loss of genetic information during replication

Question 21

Describe cross-link DNA damage

Answer 21

Covalent link formed between nucleotides. Can be:

• intrastrand: between neighboring nucleotides
• interstrand: between opposite nucleotides

Question 22

What happens if cross-link DNA damage goes unrepaired?

Answer 22

Can cause stalling of replication forks resulting in loss in genetic material

Question 23

Why is important to protect DNA in non-dividing and dividing cells?

Answer 23

Nondividing: damages accumulate
Dividing: block DNA replication, fixed as mutation which can be passed onto daughter cells, may result in cancer

Question 24

What are the 3 things that may happen to a cell with accumulated DNA damage?

Answer 24

Becomes senescent, apoptotic, or cancerous

Question 25

What happens if an error is detected by the complex signalling networks?

Answer 25

Cell cycle arrest initiated
DNA repaired by DNA pathway repairs
Transcriptional program activation or apoptosis

Question 26

At which cell cycle checkpoints is damaged detected?

Answer 26

G1, S, and G2

Question 27

What happens if DNA damage is detected at the cell cycle checkpoints?

Answer 27

ATM and ATR kinases are activated rapidly by phosphorylation. These transmit signal to proteins (eg ChK1, ChK2, p53) which activate other proteins that cause cell cycle arrest

Question 28

Which proteins detect damage at cell cycle checkpoints?

Answer 28

ATM and ATR kinases

Question 29

Why is arresting the cell cycle a good idea when DNA damage is detected?

Answer 29

More time allowed for DNA repair and activation of apoptotic pathway if damage is too great to be reapired

Question 30

Which protein pathway fixes bulky adducts and pyramadinie dimers?

Answer 30

Nucleotide excision repair

Question 31

What type of DNA damage is fixed by base excision repair?

Answer 31

Abasic site single-strand breaks

Question 32

Which repair pathway fixes base pair mismatch?

Answer 32

Mismatch repair, MMR

Question 33

What type of damage is repaired by homologous recombination repair, HRR, or non-homologous end-joining, NHEJ?

Answer 33

Double-strand breaks and interstrand crosslinks

Question 34

Which repair pathway fixes guanine alkylation?

Answer 34

Methyl-guanine methyl-transferase pathways, MGMT

Question 35

Describe what happens when DNA polymerase makes a mistake

Answer 35

DNA polymerase will make a mistake every 1/100,000 nucleotides
The wrong nucleotide is inserted, causing insertion/deletion mutations
Proof-reading corrects majority of mistakes, however mismatch repair is also used
The wrong base is removed and DNA extension is attempted again with correct base

Question 36

Describe the sequence of events involved in mismatch repair

Answer 36

MutS protein binds to mismatched base and recruits MutL protein & endonuclease which degrees faulty strand past mismatch
PCNA helps direct action
RPA binds to single strand and is copied by replicative polymerase.
Strands are sealed by ligaments.

Question 37

List the proteins involved in mismatch repair

Answer 37

MutS
MutL
Exonuclease
PCNA (proliferating cell nuclear antigen)
RPA (replicative protein A)
Replicative polymerase
Ligase

Question 38

Describe the action of direct reversal repair using methylated guanine as an example

Answer 38

Guanine is methylated on the O6 position (=> O6methylguanine)
MGMT accepts methyl group which prevents O6MeG from pairing with thymine instead of cytosine in replication

Question 39

List the five core steps of base excision repair in order

Answer 39

• Excision of base
• Incision of strand
• Processing of ends
• Repair synthesis
  [- gap filling and ligation]

Question 40

Describe how base excision repair is used to repair oxidative damage to bases

Answer 40

Damage base is removed by DNA glycosylase
Excision of base results in an AP site (apurinic or apyrimidinic)
Incised by AP endonuclease (APE1) to create single strand break
PARP1 binds to break (creating intermediate) and helps to recruit other DNA repair factors
DNA polymerase beta adds correct complementary base and DNA ligase III seals end

Question 41

What happens if ends are not processed and are resistant during base excision repair?

Answer 41

DNA polymerase adds a run of nucleotides between 2-6 and FEN1/PCNA excises flap structure
DNA ligase I seals ends

Question 42

What are the differences between short patch and long patch base excision repair?

Answer 42

Short patch uses ligase III to seal ends ad long patch uses ligase I
Long patch requires DNA polymerase to add a run of nucleotides and FEN1/PCNA to excise flap structure.
Ends can be processed in short patch but not long patch

Question 43

LIst the proteins involved in base excision repair (both long and short patch)

Answer 43

DNA glycosylase
AP endonuclease (APE1)
PARP1
Polymerase beta
DNA ligase III [short patch]
DNA polymerase [long patch]
FEN1 [long patch]
PCNA [long patch]
DNA ligase I [long patch]

Question 44

As well as oxidative damage to bases, what else can base excision repair be used to repair?

Answer 44

AP sites and strand breaks

Question 45

What are the two types of nucleotide excision repair and what is the difference?

Answer 45

Transcription coupled NER: repairs lesions on coding strand
Global genome NER: repairs rest of genome
There are differences in initial step of pathway.

Question 46

Describe the nucleotide excision repair pathway

Answer 46

Lesion is recognised by CSA and CSB in transcription coupled NER and is recognised by XPE, RAD23B and DPB in global genome NER.
TFIIH removes single stranded DNA segment which contains damage (via XPG and ERCC1XPF)
DNA polymerase uses undamaged DNA for template to replace excised strand, PCNA often acts as a cofactor for polymerase.
Ligase III joins DNA strands together

Question 47

Why are double stranded break repairs considered the most important repair pathway?

Answer 47

There is a risk of deleting genetic information if it is not repaired

Question 48

What are the two most common pathways which fix double strand breaks?

Answer 48

Homologous recombination (HR)
Non-homologous end-joining (NHEJ)

Question 49

Describe the pathway of non-homologous end-joining

Answer 49

Ku recognizes and binds to DNA ends, and then recruits subunit DNA protein kinase (PKcs)
Ends are processed via nucleuses (eg Artemis) OR DNA nucleotides are added to make ends compatible
XRCC4, Ligase IV, and XLF complex seals break

Question 50

Why is NHEJ considered error prone?

Answer 50

Small additions/deletions may occur

Question 51

Describe how homologous repair is used to fix double stranded breaks

Answer 51

During DNA replication, sister chromatids are used as a template
MRN CTIIP complex generate single strand of DNA which replication protein A (RPA) binds to
RAD51 nucleoprotein filaments search or identical sequence on homologous template, invades template, and uses correct sequence
The DNA is copied and used to mend strand, repairs are completed by joining strands

Question 52

What are the differences between NHEJ and HR

Answer 52

HR uses identical sequence from sister chromatids
NHEJ occurs throughout ll of cell cycle
HR only occurs in S and G2 phases

Question 53

Why is the balance o DNA repair important?

Answer 53

Too little repair and mutations accumulate which cause genetic instability
Too much repair and the apoptotic pathway is inhibited which may enable cells with badly damaged DNA to attempt to repair, but instead misrepair and survive

Question 54

What are 2 examples of real life situations we know cause DNA damage and cancer?

Answer 54

• UV light & skin cancer: pyramidne bases absorb UV light making them more reactiv towards other bases, forming dimers (repaired by nucleotide excision pathway)
• Smoking & lung cancer: carcinogens cause bulky adducts that bind to DNA, also contains free radicals causing oxidative damage. P53 mutations in lung cancer

Question 55

What is an example of a bacterial infection that causes cancer?

Answer 55

H Pylori, associated with stomach cancer.

Causes chronic inflammation which increases Reactive Oxidative Species, causing DNA damage

Question 56

What is an example of a viral infection that causes cancer?

Answer 56

Hepatitis B and C

Causes chronic inflammation which increases ROSs, causing DNA damage

Question 57

What % of cancers are associated with infections?

Answer 57

~10-15%

Question 58

What is functional redundancy?

Answer 58

The idea that if the main pathway for a type of DNA damage doesn’t repair the damage, a second pathway i usually available to act as backup mechanism

Question 59

List some syndromes associated itch germline mutations in DNA damage

Answer 59

Li Fraumeni
Cockayne’s
Xeroderma Pigemtosum
Franconi’s
Hereditary breast/ ovarian cancer
Hereditary no polyposis colorectal cancer
Nijemegan breakage
Altaxia talagiactasia
Bloom, Werner, Rotham, Thompson

Question 60

What can genetic instability result in?

Answer 60

Mutations
Tumour progression
Pathogenesis
Resistance to treatment

Question 61

What are mutations?

Answer 61

Permanent changes to DNA sequence

Question 62

What causes mutations?

Answer 62

Damage to DNA

Errors in replication

Question 63

What are the possible effects of mutation?

Answer 63

Prevent proteins from being expressed
Change function of proteins
Cause over-expression/activation of protein

Question 64

What are the 4 main forms of mutations?

Answer 64

Single nucleotide variants
Insertions/deletions
Aneuploidy
Microsatellite instability

Question 65

What is a single nucleotide variant?

Answer 65

A point mutation where one base is changed in an amino acid

Question 66

What happens if a single nucleotide variant mutation occurs in a DNA binding domain?

Answer 66

Affects p53 confirmation

Downstream signalling is altered

Question 67

What is the most common single nucleotide variant mutation in cancer?

Answer 67

P53

Question 68

What is an insertion mutation?

Answer 68

Extra DNA added to gene

Might be to/from a different chromsome

Question 69

What is a deletion mutation?

Answer 69

DNA removed from gene, entire gene is missing, or chromosome breaks and information is lost

Question 70

What may insertion/deletion mutations result in?

Answer 70

amplification of oncogenes

Deletion of TSGs

Question 71

What is an inversion mutation?

Answer 71

Where a chromosome breaks in two places, flips the piece, and re-inserts it back into the chromosome

Question 72

What is a translocation mutation?

Answer 72

Where a piece of chromosome breaks off and attaches to the end of chromosome

Question 73

What is an example of a translocation mutation and what part of the chromosome(s) does it affect?

Answer 73

chronic myeloid leukemia (CML)
Section of chromosome 9 containing ABL breaks and attaches to chromosome 22, creating product BCR-ABL (which is an oncogenic tyrosine kinase)

Question 74

What is Aneuploidy?

Answer 74

The addition/deletion of whole chromosomes

Question 75

What happens if the mitosis checkpoints that ensure chromosome segregation goes wrong?

Answer 75

Misregulation of chromosomes
Abnormal number of chromosomes proudiced in daughter cells
May promote cell growth / tumour genesis

Question 76

What are microsatellites?

Answer 76

Repeated DNA sequences spread throughout genome

Question 77

Generally, how many base pairs make up a microsatellite?

Answer 77

Around 1-6

Question 78

What is a genetic fingerprint?

Answer 78

The length and locus of an individual’s microsatellites

Question 79

What is microsatellite instability?

Answer 79

When microsatellites are not coherent within the individual

Question 80

What causes microsatelite instability?

Answer 80

The repeating units cause slipping during replication, resulting in insertions/deletions

Question 81

What is an example of a cancer caused by microsatellite instability?

Answer 81

Colorectal cancer

Question 82

What advantages do mutations have fr cancer cells?

Answer 82

Increase proliferation
Decrease apoptosis
Result in genetic instability
Affect all hallmarks of cancer

Question 83

Why are certain parts of genome more mutation prone?

Answer 83

Different genes have different mutation rates

Question 84

What are some examples of genes mutated in cancer?

Answer 84

P53
Rb (a TSG)
Ras and EGFR (oncogenes)

Question 85

What is a ‘caretaker’ gene?

Answer 85

A first mutation in a DNA damage and response gene which results in further mutations occurring rapidly

Question 86

Describe intra-tumour heterogeneity

Answer 86

A tumour with different mutations within in it

One part of the tumour may be different to another part depending on the mutations that occur there