DNA repair disorders 2 Flashcards
XP variant form
20% of XP patients Cells are highly UV mutable NER proficient Delayed replication of damaged DNA Defective in DNA pol n (eta) DNA pol n replicates CPDs (past T-T CPDs error free)
XPV and skin cancer
Most UV damage removed by NER
Remaining damage (mostly CPDs) cannot be replicated by pol delta/epsilon
XP-V cells lack pol n so no mechanism to replicate CPDs
Accumulate mutations at di-pyrimidic sites in TSGs
Alternative translesion polymerases
UV signature mutations in XPV
Absence of pol n leads to alternative TLS. Mis-insertion opposite damage
DNA pol zeta extends beyond addition of first base (error free)
Replication (DNA pol delta/e) leads to C to A or T to T transversion
Cockayne syndrome
Autosomal recessive Severe developmental disorder Low birthweight, growth failure Deficient neurological development No UV-induced skin cancer
Cellular features of CS
Cells sensitive to killing by UV/ other damaging agents
Normal incision at pyrimidine dimers and repair synthesis
Deficient recovery of semi-conservative DNA synthesis
Defective recovery of RNA synthesis
Defective TC-repair
GGR
Global genome repair
Slow repair of damage throughout the genome
Damage recognition by XPC/E recruits repair machinery
Specificity dependent on XPC/E
Prevents mutations
Transcription coupled repair
Fast repair of damage in transcribed strand of active genes
Stalling of RNA pol II at damage recruits machinery
Broad specificity
Functions mainly to prevent cell death
CSA/B
Transcription-repair coupling proteins
Mutated in 90% of CS patients
CSA protein interacts with RNA pol II, TFIIH and CSB
CSB (SWI/SNF protein) associates with RNA pol II, TFIIH and PARP
CS and lack of skin cancer predisposition
CS-A and CS-B cells are defective in TC-repair
RNA pol II stalls at damage. Signals for apoptosis pathway
Global genome repair normal (proliferating tissue)
No mutation accumulation as GGR repairs damage in proliferating tissue
Developmental disorder in CS
Partly explained by defect in TCR
Neural tissue is vulnerable to endogenous ROS damage
TCR normally upregulated in neural tissue
CS cells are deficient in TCR of oxidative DNA damage
Blockage of RNA pol leads to apoptosis
XP and neurological abnormalities
20 to 30% of XP patients
XP-A,B,D,F,G defective in TCR and GGR
Neural cells generate ROS which damage DNA. Damage persists and leads to apoptosis
Lynch syndrome /HNPCC
Hereditary non-polyposis colorectal carcinoma
2-3% of al colorectal cancers
Predisposition is inherited as autosomal dominant
Increased risk of other cancers
HNPCC cell features
Microsatellite instability (MSI)
Usually stable within one individual
100-1000 fold increase in mutation rates in HNPCC cells than normal cells
Mutations in MMR genes (mismatch repair) result in instability
MMR protein complexes
5 MutS homologues (hMSH2-6)
4 MutL (hMLH1-4)
90% of HNPCC mutations in hMSH2 or hMLH1
MutSalpha recognises mismatch and binds ATP. Recruits MutL-alpha.
Locates exonuclease/polymerase complex
MutS-beta recognises loop resulting from replication slippage
DNA MMR genes
Two mutations required for MSI
1st in germ-line (inherited predisposition)
Normal MS stability until loss of wt allele or epigenetic changes
Failure to repair insertions/deletions (normally by MMR) leads to mutations
Signal transduction, apoptosis, transcription regulation, DNA repair genes contain MS
