2. DNA and its mutation
• Components of DNA has its unique structures.
• Its integrity and stability are essential for life.
• Some factors can influence on DNA, resulting DNA
damage.
• If not repaired, will lead to mutation and possibly
disease.
• Permanent change in the DNA sequence is called
Mutation.
Clancy, S. (2008) DNA damage and repair: mechanisms for maintaining DNA integrity. Nature Education 1(1):103
4. Spontaneous Mutations
• Arise from errors in replication process and
base modifications
• Due to natural (biological) chemical
processes
• Base modificatons (spontaneous lesions)
– Depurination
– Deamination
• Errors in DNA replication
– Base substitution
– Base insertion and deletion
5. Depurination
• Loss of a purine base, occurs spontaneously
• A mammalian cell loses about 10,000 purines in
20hrs cell generation period
6. Depurination produces an Apurinic site
http://www.nature.com/scitable/content/depurination-produces-an-apurinic-site-55400
8. Errors in DNA replication
Base Substitutions
• No chemical reaction is perfect
• Error in replication can occur when an illegitimate
nucleotide pair (e.g. A-C) forms in DNA synthesis.
• leading to a base substitution.
9. Base insertion and deletion
Griffiths et al (2004)
Deletion
Insertion
Indel mutation
10. Induced Mutations
• Arise after treatment with mutagens or
environment agents.
• Chemicals
– Alkylating agents (ENU)
– Methylating agents (EMS)
– Polycyclic hydrocarbons
– DNA intercalating agents (ethidium bromide)
– DNA crosslinker (platinum)
– Oxidative damage (oxygen radicals)
14. Mutation and genetic disorders
Progeria
• Autosomal recessive disorders
• rapid aging disease
• caused by single point mutation
(in LMNA gene)
• Thin, bald, old-looking skin
15. Mutation and
haematological disorders
• Sickle cell anaemia
• a result of single nucleotide
polymorphism (SNP)
• Hb S
http://evolution.berkeley.edu/evolibrary/article/mutations_06
16. Mutation and Cancer
• Mutation in p53 tumor suppressor gene is the most
prevalent mutation found in human cancers (over
50%)
• P53 function – cell cycle regulation and apoptosis
induction
17. Mutated p53 and cancer
https://voer.edu.vn/m/cancer-and-the-cell-cycle/3962112d
18. Mutation in p53 gene
http://bio1151.nicerweb.com/Locked/media/ch18/p53_tumor-suppressor.html
20. DNA Repair
• Restore the premutational damage to the normal
base sequence
• Failure in these systems can lead to a higher
mutation rate
• Some repair systems are very efficient at resorting
the original sequence.
• Others convert the original sequence into a
permanent mutation.
21. DNA Repair (Cont’d)
• Repair the damaged DNA base
• Delete the damaged DNA and using the
complementary sequences to restore the normal
sequence
Direct reversal
Excision repair pathways
Repair of double strand breaks
22. Direct reversal of damaged DNA
• Photoreactivation by
Photolyase enzyme.
23. Base Excision Repair (BER)
• Repair of AP sites
glycosylase
AP endonuclease
Excision exonuclease
DNA polymerase
DNA ligase
Griffiths et al (2004)
24. Nucleotide Excision Repair
(NER)
Excinuclease
• detects the distortions in
double helix cause by the
presence of abnormal base
• Such distortions include
pyrimidine dimer caused by
UV light or aflatoxin induced
mutation.
Griffiths et al (2004)
25. Repair of double-strand breaks
• Double-strand break is a mutation in which both
strands of the double helix were to break at sites that
were close together.
• If left unrepaired, this can cause a variety of
chromosomal aberrations resulting in cell death or a
precancerous state.
• Double-strand breaks can arise spontaneously or
induced by ionizing radiation.
• Two mechanisms to repair these lesions are
Nonhomologous end joining (NHEJ) and homologous
recombination.
26. Nonhomologous end-joining
(NHEJ)
• Complementary strand cannot
exploited because both strands
are damage.
• No sister chromatid
• Error prone mechanism
• Imperfect repair
• Better than leaving unrepaired
Griffiths et al (2004)
28. Human disease and DNA repair defect
Disease Cancer susceptibility Symptoms
Ataxia
telangiectasia
Lymphomas Telangiectases in skin
and eyes, immune
dysfunction
Bloom syndrome Carcinomas, leukaemias,
Lymphomas
Facial telangiectases,
photosensitivity
Fanconi anemia Leukaemias pancytopenia
Xeroderma
pigmentosum
Skin carcinomas, melanomas Skin and eye
photosensitivity,
keratoses
http://www.ncbi.nlm.nih.gov/books/NBK21794/table/A2780/?report=objectonly
29.
30. PTEN
• Phosphatase and tensin homolog detected on
chromosome Ten
• Tumor suppressor protein
• play a role in maintenance of tumor
microenvironment, cellular senescence and cell cycle
regulation
• regulate DNA damage mechanism
32. Objectives of the study
• To investigate the role of phosphorylation
• subsequent nuclear localization of PTEN with DNA
repair.
• Using PTEN deficient U87MG cells
33. Materials and Methods
• MTT assay
• Fluorescence microscopy
• Western blotting and immunoprecipitation
• Comet assay
• Statistical analysis with Origin Pro v.8 software
34. Results from MTT assay
Percentage of survivability is lowered in all transfected cells compared to untransfected cell
37. Conclusion
• DNA damage augments phosphorylation of PTEN.
• Nuclear accumulation of PTEN increases which
positively regulates the DNA repair process.
• PTEN as the intermediate component of DNA repair.
• Phosphorylation of PTEN is associated with DNA
repair
• PTEN is essential for successful DNA repair.
38. References
• Clancy S. DNA damage and repair: Mechanisms for
Maintaining DNA Integrity. Nature Education.
2008;1(1):103.
• Griffiths AJF, Wessler SR, Lewontin RC, Gelbart WM,
Suzuki DT, Miller JH. Introduction to Genetic Analysis. 8th
ed. W.H. Freeman; 2004.
• Karp G. Cell and Molecular Biology: Concepts and
Experiments. 7th ed. John Wiley and Sons Inc; 2013.
• Wei, S., Shalhout, S., Ahn, Y.H. and Bhagwat, A.S. (2015).
A versatile new tool to quantify abasic sites in DNA and
inhibit base excision repair. DNA repair 27(2015)9-18