1. 1 GENE MUTATION�AND DNA REPAIR Chapter 16
2. 2 GENETIC MATERIAL DNA
Primary function permanent storage of information
Does not normally change
Mutations do occur
3. 3 MUTATIONS Mutation
Heritable change in the genetic material
Permanent structural change of DNA
Alteration can be passed on to daughter cells
Mutations in reproductive cells can be passed to offspring
4. 4 MUTATIONS Mutations
Provide allelic variation
Ultimate source of genetic variation
Foundation for evolutionary change
Various phenotypic effects
Neutral
Harmful
Beneficial
5. 5 MUTATIONS Mutations
Most mutations are neutral
More likely to be harmful than beneficial to the individual
More likely to disrupt function �than improve function
6. 6 MUTATIONS Mutations
Many inherited diseases result from mutated genes
Diseases such as various cancers can be caused by environmental agents known to �cause DNA mutations
Mutagens
7. 7 MODEL ORGANISMS Much of our understanding of mutations is a result of the study of model organisms
e.g., Bacteria, yeast, Drosophila, etc.
Amenable to analysis
Short generation time, numerous offspring, etc.
Often exposed to mutagenic environmental agents
Effects of mutations are studied
8. 8 TYPES OF MUTATIONS Types of mutations
Chromosome mutations
Changes in chromosome structure
Genome mutations
Changes in chromosome number
Single-gene mutations
Relatively small changes in DNA �structure
Occur within a particular gene
Focus of study in this chapter
9. 9 TYPES OF MUTATIONS Mutations involve the permanent alteration of a DNA sequence
Alteration of base sequence
Removal or addition of one or more nucleotides
10. 10 MUTATIONS Point mutations
Change in a single base pair within the DNA
Two main types of point mutations
Base substitutions
Transition
Transversion
Small deletions or insertions
11. 11 MUTATIONS Two types of base substitutions
Transition
Pyrimidine changed to another pyrimidine
e.g., C ? T
Purine changed to another purine
e.g., A ? G
Transversion
Purines and pyrimidines are �interchanged
e.g., A ? C
More rare than transitions
12. 12 EFFECTS OF MUTATIONS Mutations within the coding sequence of a gene can have various effects on the encoded polypeptides amino acid sequence
Silent mutations
Missense mutations
Included neutral mutations
Nonsense mutations
Frameshift mutations
13. 13 EFFECTS OF MUTATIONS Silent mutations
Amino acid sequence is not altered
e.g., CCC ? CCG (pro ? pro)
Genetic code is degenerate
Alterations of the third base of a codon often do not alter the encoded amino acid
Phenotype is not affected
14. 14 EFFECTS OF MUTATIONS Missense mutations
Amino acid sequence is altered
e.g., GAA ?GTA (glu ? val)
Phenotype may be affected
15. 15 EFFECTS OF MUTATIONS Neutral mutations
Type of missense mutation
Amino acid sequence is altered
e.g., CTT ?ATT (leu ? ile)
e.g., GAA ?GAC (glu ? asp)
No detectable effect on protein function
Missense mutations substituting an amino acid with a similar chemistry to the original is likely to be neutral
16. 16 EFFECTS OF MUTATIONS Nonsense mutations
Normal codon is changed into a stop �codon
e.g., AAA ? AAG (lys ? stop)
Translation is prematurely terminated
Truncated polypeptide is formed
Protein function is generally affected
17. 17 EFFECTS OF MUTATIONS
18. 18 EFFECTS OF MUTATIONS
19. 19 EFFECTS OF MUTATIONS Mutations occasionally produce a polypeptide with an enhanced ability to function
Relatively rare
May result in an organism �with a greater likelihood �to survive and reproduce
Natural selection may �increase the frequency of �this mutation in the �population
20. 20 MUTATION TYPES Genetic terms to describe mutations
Wild-type
Relatively common genotype
Generally the most common allele
Variant
Mutant allele altering an organisms phenotype
Forward mutation
Changes wild-type allele into something else
Reverse mutation
Reversion
Restores wild-type allele
21. 21 MUTATION TYPES Genetic terms to describe mutations
Deleterious mutation
Decreases an organisms chance of �survival
Lethal mutation
Results in the death of an organism
Extreme example of a deleterious �mutation
Conditional mutants
Affect the phenotype only under a �defined set of conditions
e.g., Temperature-sensitive (ts) mutants
22. 22 MUTATION TYPES Genetic terms to describe mutations
Suppressor mutation
Second mutation that restores the wild-type phenotype
Intragenic suppressor
Secondary mutation in the same gene as �the first mutation
Differs from a reversion
Second mutation is at a different site �than the first
Intergenic suppressor
Secondary mutation in a different gene �than the first mutation
23. 23 MUTATION TYPES Two general types of intergenic suppressors
Those involving an ability to defy the genetic code
Those involving a mutant structural gene
24. 24 MUTATION TYPES Intergenic suppressor mutations involving an ability to defy the genetic code
e.g., tRNA mutations
Altered anticodon region
e.g., Recognize a stop codon
May suppress a nonsense mutation �in a gene
May also suppress stop codons �in normal genes
25. 25 MUTATION TYPES Intergenic suppressors involving a mutant structural gene
Usually involve altered expression of one gene that compensates for a loss-of-function mutation affecting another gene
Second gene may take over the functional role of the first
May involve proteins participating in a common cellular function
Sometimes involve mutations in genetic regulatory proteins
e.g., Transcription factors activating other genes that can compensate for the mutation in the first gene
26. 26 MUTATION TYPES Mutations occurring outside of coding sequences can influence gene expression
Mutations may alter the core promoter sequence
Up promoter mutations
Mutant promoter becomes more like the consensus sequence
Rate of transcription may be increased
Down promoter mutations
Mutant promoter becomes less like the consensus sequence
Affinity for regulatory factors is decreased
Rate of transcription may be decreased
27. 27 MUTATION TYPES Mutations occurring outside of coding sequences can influence gene expression
Mutations may alter other regulatory sequences
lacOC mutations prevent binding of �the lac repressor
Lac operon is constituently expressed, �even in the absence of lactose
Such expression is wasteful
Such mutants are at a selective �disadvantage
28. 28 MUTATION TYPES Mutations occurring outside of coding sequences can influence gene expression
Mutations may alter splice junctions
Altered order and/or number of exons in the mRNA
29. 29 MUTATION TYPES Mutations occurring outside of coding sequences can influence gene expression
Mutations may affect an �untranslated region of mRNA
5- or 3-UTR
May affect mRNA stability
May affect the ability of the �mRNA to be translated
30. 30 MUTATION TYPES
31. 31 TRINUCLEOTIDE REPEATS DNA trinucleotide repeats
Three nucleotide sequences repeated in tandem
e.g., CAGCAGCAGCAGCAGCAG
Generally transmitted normally from parent to offspring without mutation
32. 32 TRINUCLEOTIDE REPEATS Trinucleotide repeat expansion (TNRE)
Number of repeats can readily increase from one generation to the next
Cause of several human genetic �diseases
Length of a repeat has increased �above a certain critical size
Becomes prone to frequent �expansion
33. 33 TRINUCLEOTIDE REPEATS TNRE disorders
Fragile X syndrome (FRAXA)
FRAXE mental retardation
Myotonic muscular dystrophy (DM)
Spinal and bulbar muscular atrophy (SBMA)
Huntington disease (HD)
Spinocerebellar ataxia (SCA1)
34. 34 TRINUCLEOTIDE REPEATS TNRE disorders
35. 35 TRINUCLEOTIDE REPEATS TNRE disorders
Expansion may be within a coding sequence of a gene
Most expansions are of a CAG repeat
Encoded proteins possess long tracts of glutamine
CAG encodes a glutamine codon
Presence of glutamine tracts causes aggregation of the proteins
Aggregation is correlated with the progression of the disease
36. 36 TRINUCLEOTIDE REPEATS TNRE disorders
Expansion may be in a noncoding region of a gene
Two fragile X syndromes
Repeat produces CpG islands that become methylated
Methylation can lead to chromosome compaction
Can silence gene transcription
Myotonic muscular dystrophy
Expansions may cause abnormal changes in RNA structure
37. 37 TRINUCLEOTIDE REPEATS TNRE disorders
Severity of the disease tends to worsen in future generations
Anticipation
Severity of the disease depends on the parent from whom it was inherited
e.g., In Huntingdon disease, TNRE likely to occur if mutation gene is inherited from the father
e.g., In myotonic muscular dystrophy, TNRE likely to occur if mutation gene is inherited from the mother
38. 38 TRINUCLEOTIDE REPEATS TNRE disorders
39. 39 TRINUCLEOTIDE REPEATS TNRE disorders
Cause of TNRE is not well understood
Trinucleotide repeat may produce alterations in DNA structure
e.g., Stem-loop formation
May lead to errors in DNA replication
TNRE within certain genes alters gene expression
Disease symptoms are produced
40. 40 CHROMOSOME STRUCTURE Altered chromosome structure can alter gene expression
Inversions and translocations commonly have no obvious phenotypic effects
Phenotypic effects sometimes occur
Position effect
41. 41 CHROMOSOME STRUCTURE Altered chromosome structure can alter gene expression and phenotype
Breakpoint may occur within a gene
Expression of the gene is altered
Breakpoint may occur near a gene
Expression is altered when moved to a new location
May be moved next to regulatory elements influencing the expression of the relocated gene
i.e., Silencers or enhancers
May reposition a gene from a euchromatic region to a highly condensed (heterochromatic) region
Expression may be turned off
42. 42 CHROMOSOME STRUCTURE Altered chromosome structure can alter gene expression and phenotype
An eye color gene relocated to a heterochromatic region can display altered expression
Gene is sometimes inactivated
Variegated phenotype results
43. 43 SOMATIC VS. GERM-LINE The timing of mutations in multicellular organisms plays an important role
Mutations may occur in gametes or a fertilized egg
Mutations may occur later in life
Embryonic or adult stages
Timing can affect
The severity of the genetic effect
The ability to be passed from parent to offspring
44. 44 SOMATIC VS. GERM-LINE Animals possess germ-line and somatic cells
Germ-line cells
Cells giving rise to gametes
Somatic cells
All cells of the body �excluding the germ-line cells
e.g., Muscle cells, nerve cells, �etc.
45. 45 SOMATIC VS. GERM-LINE Germ-line cells
Germ-line mutations can occur in gametes
Germ-line mutations can occur in a precursor cell that produces gametes
All cells in the resulting offspring will contain the mutation
46. 46 SOMATIC VS. GERM-LINE Somatic cells
Somatic mutations in embryonic cells can result in patches of tissues containing the mutation
Size of the patch depends on the timing of the mutation
Individual is a genetic mosaic
47. 47 CAUSES OF MUTATIONS Two causes of mutations
Spontaneous mutations
Result from abnormalities in biological �processes
Underlying cause lies within the cell
Induced mutations
Caused by environmental agents
Cause originates outside of the cell
48. 48 CAUSES OF MUTATIONS Causes of spontaneous mutations
Abnormalities in crossing over
Aberrant segregation of chromosomes during meiosis
Mistakes by DNA polymerase during replication
Alteration of DNA by chemical products of normal metabolic processes
Integration of transposable elements
Spontaneous changes in nucleotide structure
49. 49 CAUSES OF MUTATIONS Induced mutations are caused by mutagens
Chemical substances or physical agents originating outside of the cell
Enter the cell and then alter the DNA structure
50. 50 CAUSES OF MUTATIONS
51. 51 CAUSES OF MUTATIONS Spontaneous mutations are random events
Not purposeful
Mutations occur as a matter of chance
Some individuals possess beneficial mutations
Better adapted to their environment
Increased chance of surviving and reproducing
Natural selection results in differential reproductive success
The frequency of such alleles increases in the population
52. 52 CAUSES OF MUTATIONS Salvador Luria and Max Delbruck
T1 is a bacteriophage able to infect E coli
A small percentage of bacteria are resistant to T1 infection
Heritable trait
tonr (T1 resistance)
Is this resistance due to spontaneous mutations or due to a physiological adaptation?
53. 53 CAUSES OF MUTATIONS Salvador Luria and Max Delbruck
The question
Is T1 resistance due to spontaneous mutations or due to a physiological adaptation?
54. 54 CAUSES OF MUTATIONS Salvador Luria and Max Delbruck
Two competing theories
Adaptation theory
Rate of adaptation should be relatively constant
Depends on exposure to bacteriophage
tonr cells should be a relatively constant proportion of the total bacterial population
Spontaneous mutation theory
Number of tonr cells is dependent on timing of mutation
tonr mutation occurring early in proliferation ? many tonr mutants found
tonr mutation occurring late in proliferation ? fewer tonr mutants found
Predicts greater variation in the number of tonr cells present in different populations
55. 55 CAUSES OF MUTATIONS Salvador Luria and Max Delbruck
The experiment
Fluctuation test
Grew T1-susceptible bacteria in a flask and in several individual tubes
Plated onto �media with T1 �phage
Counted number �of tonr colonies
56. 56 CAUSES OF MUTATIONS Salvador Luria and Max Delbruck
The results
Even distribution of tonr colonies from large flask
Great fluctuation in number of tonr colonies from small tubes
57. 57 CAUSES OF MUTATIONS Salvador Luria and Max Delbruck
The conclusion
Results are consistent with the spontaneous mutation theory
Timing of the mutation during the growth of a culture greatly affects the number of mutant cells
58. 58 CAUSES OF MUTATIONS Joshua and Ester Lederberg (1950s)
Interested in the relationship between mutation and the environmental conditions shat select for mutations
Scientists were unsure of the relationship
Two competing hypotheses
Directed mutation hypothesis
Some scientists still believed that selective conditions could promote specific mutations
Random mutation theory
Mutations occur at random
Environmental factors affecting survival select for those possessing beneficial mutations
59. 59 CAUSES OF MUTATIONS Joshua and Ester Lederberg (1950s)
Plated large number of bacteria onto a master plate
Contained no selective agent
Transferred colonies to �secondary plates containing �selective agent (T1 phage)
Replica plating
Only mutant cells would grow
60. 60 CAUSES OF MUTATIONS Joshua and Ester Lederberg (1950s)
Mutants occupied the same locations on all secondary plates
Indicated that mutations �occurred randomly in colonies �growing on the nonselective �master plate
Ransom mutation theory is �supported
61. 61 CAUSES OF MUTATIONS Mutation rate
Likelihood that a gene will be altered by a new mutation
Expressed as the number of new mutations in a given gene per generation
Generally 1/100,000 1/billion
10-5 10-9
62. 62 CAUSES OF MUTATIONS Mutation rate
Mutation rate is not a constant number
Can be increased by environmental �mutagens
Induced mutations can increase beyond �frequency of spontaneous mutations
Mutation rates vary extensively �between species
Even vary between strains of the �same species
63. 63 CAUSES OF MUTATIONS Mutation rate
Some genes mutate at a much higher rate than other genes
Some genes are longer than others
Some locations are more �susceptible to mutation
Even single genes possess mutation �hot spots
More likely to mutate than other �regions
64. 64 CAUSES OF MUTATIONS Mutation frequency
Number of mutant alleles of a given gene divided by the number of alleles within a population
Timing of mutations influences mutation frequency
Timing does not influence mutation rate
Mutation frequency depends both on mutation rate and timing of mutations
Natural selection and genetic drift can further increase mutation frequencies
65. 65 CAUSES OF MUTATIONS Spontaneous mutations: Depurination
Most common type of naturally occurring chemical change
Reaction with water removes a purine (A or G) from the DNA
Apurinic site
66. 66 CAUSES OF MUTATIONS Spontaneous mutations: Depurination
~10,000 purines lost per 20 hours at 37oC in a typical mammalian cell
Rate of loss increased by agents causing certain base modification
e.g., Attachment of alkyl �(methyl, ethyl, etc.) groups
Generally recognized by �DNA repair enzymes
Mutation may result if �repair system fails
67. 67 CAUSES OF MUTATIONS Spontaneous mutations: Deamination of cytosines
Other bases are not readily deaminated
Removal of an amino group from the cytosine base
Uracil is produced
DNA repair enzymes generally remove this base
Uracil is recognized as an inappropriate base
Mutation may result if repair system fails
Uracil hydrogen bonds with A, not G
68. 68 CAUSES OF MUTATIONS Spontaneous mutations: Deamination of cytosines
Methylation of cytosine occurs in many eukaryotic species as well as prokaryotes
Removal of an amino group from the 5-methyl cytosine produces thymine
DNA repair enzymes cannot determine which is the incorrect base
Hot spots for mutations are produced
69. 69 CAUSES OF MUTATIONS Spontaneous mutations: Tautomeric shifts
Common, stable form of T and G is the keto form
Interconvert to an enol form at a low rate
Common, stable form of A and C is the amino form
Interconvert to an imino form at a low rate
70. 70 CAUSES OF MUTATIONS Spontaneous mutations: Tautomeric shifts
Enol and imino forms do not conform to normal base-pairing rules
AC and GT base pairs are formed
71. 71 CAUSES OF MUTATIONS Spontaneous mutations: Tautomeric shifts
Tautomeric shifts immediately prior to DNA replication can cause mutations
Resulting mismatch �could be repaired
Mutation may result if �repair system fails
72. 72 CAUSES OF MUTATIONS Hermann Muller (1927)
Showed that X rays can cause induced mutations
Reasoned that a mutagenic agent might form defective alleles
Experimental approach focused on �formation and detection of X-linked �genes in Drosophila melanogaster
73. 73 CAUSES OF MUTATIONS Hermann Muller (1927)
The hypothesis
Exposure to X rays will increase the rate of mutation
74. 74 CAUSES OF MUTATIONS Hermann Muller (1927)
The materials
Drosophila melanogaster strain with three genetic alterations of the X chromosome
ClB chromosome
C: Large inversion preventing productive crossing over
l: Lethal recessive X-linked gene
B: Bar eye allele
75. 75 CAUSES OF MUTATIONS Hermann Muller (1927)
The design
Females with one ClB chromosome and one normal chromosome
Cannot undergo crossovers in the C region
Can only produce sons possessing the normal X chromosome
Lethal mutations in the normal chromosome will prevent them from producing any sons
76. 76 CAUSES OF MUTATIONS Hermann Muller (1927)
The experiment
Exposed wild-type males to X rays
May mutate the X chromosome in sperm
Mated mutagenized males to females with the ClB chromosome
Daughters with bar eyes were saved
Mated to wild-type males
Genders of offspring determined
77. 77 CAUSES OF MUTATIONS Hermann Muller (1927)
The data
78. 78 CAUSES OF MUTATIONS Hermann Muller (1927)
Interpreting the data
Very few lethal mutations occurred in the untreated control
Approximately 1 in 1,000
Many more mutations occurred in the X ray-treated flies
Nearly 100 times more
X rays greatly increase the rate of �X-linked recessive lethal mutations
79. 79 CAUSES OF MUTATIONS The public is concerned about mutagens for two important reasons
Mutagenic agents are often �involved in the development �of human cancers
Avoiding mutations that may �have harmful effects on future �offspring is desirable
80. 80 CAUSES OF MUTATIONS An enormous array of agents can act as mutagens
Chemical agents and physical agents
81. 81 CAUSES OF MUTATIONS Certain non-mutagenic chemicals can be altered to a mutagenically active form after ingestion
Cellular enzymes such as oxidases can activate some mutagens
Certain foods contain chemicals acting as antioxidants
Antioxidants may be able to counteract the effects of mutagens and lower cancer rates
82. 82 CAUSES OF MUTATIONS Mutagens alter DNA structure in various ways
Nitrous acid (HNO3) replaces amino groups with keto groups
-NH2 ? =O
Can change cytosine �to uracil
Pairs with A, not G
Can change adenine �to hypoxanthine
Pairs with C, not T
83. 83 CAUSES OF MUTATIONS Mutagens alter DNA structure in various ways
Alkylating agents covalently attach methyl or ethyl groups to bases
e.g., Nitrogen mustards, ethyl �methanesulfonate (EMS)
Appropriate base pairing is �disrupted
84. 84 CAUSES OF MUTATIONS Mutagens alter DNA structure in various ways
Some mutagens directly interfere with the DNA replication process
e.g., Acridine dyes such as proflavin
Flat, planar structures interchelate into the double helix
Sandwich between adjacent base pairs
Helical structure is distorted
Single-nucleotide additions and deletions can result
85. 85 CAUSES OF MUTATIONS Mutagens alter DNA structure in various ways
Some mutagens are base analogs
e.g., 2-aminopurine
e.g., 5-bromouracil (5BU)
Become incorporated into �daughter strands during �DNA replication
86. 86 CAUSES OF MUTATIONS Mutagens alter DNA structure in various ways
Some mutagens are base analogs
5-bromouracil (5BU) is a thymine �analog
Incorporated in place of thymine
5BU can base-pair with adenine
Can tautomerize and base-pair with �guanine at a relatively high rate
AT ? A5BU ? G5BU ? GC
Transition mutations occur
87. 87 CAUSES OF MUTATIONS Mutagens alter DNA structure in various ways
DNA molecules are sensitive to physical agents such as radiation
e.g., Ionizing radiation such as X rays and gamma rays
Short wavelength and high energy
Can penetrate deeply into biological materials
Creates free radicals
Chemically reactive molecules
Free radicals alter DNA structure in a variety of ways
Deletions, single nicks, cross-linking, chromosomal breaks
88. 88 CAUSES OF MUTATIONS Mutagens alter DNA structure in various ways
DNA molecules are sensitive to physical agents such as radiation
e.g., Nonionizing radiation such as �UV light
Contains less energy
Penetrates only the surface of material �such as the skin
Causes the formation of thymine dimers
May be repaired through one of numerous �repair systems
May cause a mutation when that DNA �strand is replicated
89. 89 CAUSES OF MUTATIONS Many different kinds of testes can determine if an agent is mutagenic
Ames test is commonly used
Developed by Bruce Ames
Uses his- strains of Salmonella typhimurium
Mutation is due to a point mutation rendering an enzyme inactive
Reversions can restore his+ phenotype
Ames test monitors rate of reversion mutations
90. 90 CAUSES OF MUTATIONS Ames test
Suspected mutagen is mixed with rat liver extract and his- Salmonella typhimurium
Rat liver extract provides cellular �enzymes that may be required to �activate a mutagen
Bacteria are plated on minimal �media
his+ revertants can be detected
Mutation frequency calculated
Compared to control
91. 91 DNA REPAIR Most mutations are deleterious
DNA repair systems are vital to the survival
Bacteria possess several different DNA repair systems
Absence of a single system greatly �increases mutation rate
Mutator strains
Humans defective in a single DNA �repair system may manifest various �disease symptoms
e.g., Higher risk of skin cancer
92. 92 DNA REPAIR Living cells contain several DNA repair systems
Able to fix different types of DNA alterations
