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Mutation Point Mutations Repair of “point” mutations

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Presentation on theme: "Mutation Point Mutations Repair of “point” mutations"— Presentation transcript:

1 Mutation Point Mutations Repair of “point” mutations
Covered Spontaneous and Induced last time Ames Test for Mutagens (because some mutagens = carcinogens) Repair of “point” mutations Transposon as mutagens

2 Example Results of the Ames Test
Ames test measures rate that mutagen reverts mutant phenotype to wild type Wild type Salmonella typhimurium can make histidine, so it can grow on medium lacking histidine (histidine protoroph). S. typhimurium mutants contain different types of mutations in a His biosynthesis gene, they cannot make histidine and cannot grow on medium lacking histidine (histidine auxotrophs). Part of wild type His+ amino acid sequence: Cys His Ala Ser Met Part of wild type His+ gene sequence: TGT CAC GCC TCT ATG TA100 [His to Arg missense (nonconserv. substitution)] TGT CGC GCC TCT ATG TA1538 [frameshift mutation] TGT TCA CGC CTC TAT G His+ revertant of TA 1538 (pseudorevertant) TGT TCC GCC TCT ATG TA w [Ser to Pro missense (nonconserv. substitution] TGT CAC GCC CCT ATG TA x [Cys to Tyr missense (noncoserv. substituion] TAT CAC GCC TCT ATG TA y [Met to Ile missense (conservative substitution] TGT CAC GCC TCT ATA TA z [Cys to Trp missense (nonconserv. substitution] TGG CAC GCC TCT ATG Possible mechanisms of mutation from His+ to His- = ? Revertants = His- strains mutated back to His+ phenotype True Revertants: change back to the wild type sequence (G back to A in TA100) Pseudorevertants: change that compensates for first mutation without fixing it (suppressor mutation) A. deletion of A in TA1538 fixes frame shift, results in a conservative substitution B. a second missense mutation in TA100 ( TA x or TA y or TA z) that allows protein to fold properly C. a mutation in a different gene - not relevant to Ames test.

3 Repair Processes Direct Reversal of DNA lesion
photolyase repair of UV lesions alkyltransferase repair of alkylations Homology-dependent repair processes Pre-replication repair General nucleotide excision repair of bulky lesions pyrimidine dimers, insertion or deletions loops defects cause Xeroderma pigmentosa Nucleotide excision repair starting with specific glycosidases specific base modifications, removal of Uracil Post-replication repair Mismatch repair Defects cause Hereditary Nonpolyposis Colon Cancer DNA replication at sites of DNA damage Recombinational repair (error free) SOS system (error prone)

4 Light-dependent repair by photolyase
When inducing mutations using UV – keep cells in the dark until after DNA replication in order to avoid this

5 Base-excision repair Base-excision repair and general nucleotide excision repair are similar after the initial steps Both involve exonucleolytic removal of many nucleotides on either side of the lesion General nucleotide excision repair can remove bulky lesions pre-replication Base-excision repair differs in that more subtle lesions can be recognized - C to U by deamination - damaged bases - each base is removed by a specific glycosylase - then AP endonuclease… - then exonucleolytic removal and fill in synthesis – see next slide

6 Base-excision repair

7 Mismatch excision repair
Mutations in mismatch repair genes contribute to development o f colon cancer Mismatch is repaired to the correct sequence by recognizing methylated vs nonmethylated DNA Step 3 and 4 are similar to other excision repair pathways

8 Assay of UV sensitivity of cells cultured from Xeroderma Pigmentosa patients
Each cell line is a different complementation group - complementation groups defined by testing heterokaryons for UV sensitivity - if a heterokaryon made by fusing Cell A with Cell B (A B heterokaryon) is UV sensitive, then A and B have mutations in the same comp. group (same gene). - if heterokaryon is no longer UV sensitive, then mutations are in different complementation groups (different genes) Many of these mutation have been mapped to a unique chromosomal location, confirming different complementation groups = different genes Genes identified with XP groups related to excision repair genes important for removing pyrimidine dimers due to UV light.

9 Getting past a replication block by Recombinational Repair
RecA protein recognizes ss DNA region skipped during replication Can’t use damaged strand as template Promotes recombination event removing strand from other replication fork Template exists to replace this stand of DNA Lesion causing the block is still present and must be removed (excision repair)

10 Error-prone SOS-mediated repair
If block to replication is not fixed by recombinational repair – then repair or die pathway kicks in – SOS repair when SOS vs recombinational? High levels of damage, defects in recombination repair… Random sequence is added to the new strand opposite the DNA lesion

11 Transposons as mutagens
ALSO: Insertion of TN near a Gene can cause Change regulation Of gene expression different from inactivation of regulatory sequence here, adding new regulatory sequences (from the TN) For example, can cause gene to be expressed in cell types that normally do not express the gene – gain of function mutation

12 Transposons DNA transposons TNs Retrotransposons
Transpose through DNA – no RNA intermediate Contain inverted repeat sequences at end Autonomous TNs encode transposase Mechanims of transposion: conservative or replicative 10-20 bps are duplicated at the site of insertion Can identify sites of TN insertions even when TN is no longer there Nonautonomous TNs contain repeats but don’t encode active transposase Retrotransposons Transpose through an RNA intermediate (require reverse transcriptase) Contain direct repeats at ends that contain transcriptional signals Can be autonomous or nonautonomous Major class of TNs in human genome

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14 Example showing duplication of “target site” = site of insertion

15 Transposons (repetitive DNA elements)
Mobile Genetic Elements in Humans DNA transposons transpose either by conservative or replicative mechanism many defective copies exist most (all?) are now inactive retrotransposons (move by reverse transcription) LINEs (long interspersed elements) 6 to 8 kb, 20 to 40 thousand copies/genome Autonomous elements encode all proteins required for transposition SINEs (short interspersed elements) Deletion derivates from LINEs Alu elements (AluI = restriction enzyme site) similar to 7SL RNA = part of SRP Pseudogenes SINEs, Alu, and pseudogenes are thought to use reverse transposition proteins of LINE elements Autonomous vs Nonautonomous Transposition autonomous transposons encode their own transposition enzymes One type of LINE element in humans is still active - example of a hemophilia caused by an apparent + of a LINE element into a X-linked blot clotting factor gene during gametogenesis in a woman An active SINE element = Alu element -

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