Title: Summary of sixth lesson
1Summary of sixth lesson
- Janzen-Connol hypothesis explanation of why
diseases lead to spatial heterogeneity - Diseases also lead to heterogeneity or changes
through time - Driving succession
- The Red Queen Hypothesis selection pressure will
increase number of resistant plant genotypes - Co-evolution pathogen increase virulence in
short term, but in long term balance between host
and pathogen - Complexity of forest diseases primary vs.
secondaruy, modes of dispersal etc
2HOST-SPECIFICITY
- Biological species
- Reproductively isolated
- Measurable differential size of structures
- Gene-for-gene defense model
- Sympatric speciation Heterobasidion, Armillaria,
Sphaeropsis, Phellinus, Fusarium forma speciales
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4Phylogenetic relationships within the
Heterobasidion complex
Fir-Spruce
Pine Europe
Pine N.Am.
5Recognition of self vs. non self
- Intersterility genes maintain species gene pool.
Homogenic system - Mating genes recognition of other to allow for
recombination. Heterogenic system - Somatic compatibility protection of the
individual.
6INTERSTERILITY
- If a species has arisen, it must have some
adaptive advantages that should not be watered
down by mixing with other species - Will allow mating to happen only if individuals
recognized as belonging to the same species - Plus alleles at one of 5 loci (S P V1 V2 V3)
7MATING
- Two haploids need to fuse to form nn
- Sex needs to increase diversity need different
alleles for mating to occur - Selection for equal representation of many
different mating alleles
8SEX
- Ability to recombine and adapt
- Definition of population and metapopulation
- Different evolutionary model
- Why sex? Clonal reproductive approach can be very
effective among pathogens
9Long branches in between groups suggests no sex
is occurring in between groups
Fir-Spruce
Pine Europe
Pine N.Am.
10Small branches within a clade indicate sexual
reproduction is ongoing within that group of
individuals
NA S
NA P
EU S
890 bp CIgt0.9
EU F
11SOMATIC COMPATIBILITY
- Fungi are territorial for two reasons
- Selfish
- Do not want to become infected
- If haploids it is a benefit to mate with other,
but then the nn wants to keep all other
genotypes out - Only if all alleles are the same there will be
fusion of hyphae - If most alleles are the same, but not all, fusion
only temporary
12The biology of the organism drives an epidemic
- Autoinfection vs. alloinfection
- Primary spreadby spores
- Secondary spreadvegetative, clonal spread, same
genotype . Completely different scales (from
small to gigantic) - Coriolus
- Heterobasidion
- Armillaria
- Phellinus
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14OUR ABILITY TO
- Differentiate among different individuals
(genotypes) - Determine gene flow among different areas
- Determine allelic distribution in an area
15WILL ALLOW US TO DETERMINE
- How often primary infection occurs or is disease
mostly chronic - How far can the pathogen move on its own
- Is the organism reproducing sexually? is the
source of infection local or does it need input
from the outside
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22Evolution and Population genetics
- Positively selected genes
- Negatively selected genes
- Neutral genes normally population genetics
demands loci used are neutral - Loci under balancing selection..
23Evolution and Population genetics
- Positively selected genes
- Negatively selected genes
- Neutral genes normally population genetics
demands loci used are neutral - Loci under balancing selection..
24Evolutionary history
- Darwininan vertical evolutionray models
- Horizontal, reticulated models..
25Phylogenetic relationships within the
Heterobasidion complex
Fir-Spruce
Pine Europe
Pine N.Am.
26Geneaology of S DNA insertion into P ISG
confirms horizontal transfer.Time of
cross-over uncertain
NA S
NA P
EU S
890 bp CIgt0.9
EU F
27Because of complications such as
- Reticulation
- Gene homogeneization(Gene duplication)
- Need to make inferences based on multiple genes
- Multilocus analysis also makes it possible to
differentiate between sex and lack of sex
(Iaindex of association)
28Basic definitions again
- Locus
- Allele
- Dominant vs. codominant marker
- RAPDS
- AFLPs
29How to get multiple loci?
- Random genomic markers
- RAPDS
- Total genome RFLPS (mostly dominant)
- AFLPS
- Microsatellites
- SNPs
- Multiple specific loci
- SSCP
- RFLP
- Sequence information
- Watch out for linked alleles (basically you are
looking at the same thing!)
30Sequence information
- Codominant
- Molecules have different rates of mutation,
different molecules may be more appropriate for
different questions - 3rd base mutation
- Intron vs. exon
- Secondary tertiary structure limits
- Homoplasy
31Sequence information
- Multiple gene genealogiesdefinitive phylogeny
- Need to ensure gene histories are comparable
partition of homogeneity test - Need to use unlinked loci
32DNA template
Reverse primer
Forward primer
Thermalcycler
33Gel electrophoresis to visualize PCR product
Ladder (to size DNA product)
34From DNA to genetic information (alleles are
distinct DNA sequences)
- Presence or absence of a specific PCR amplicon
(size based/ specificity of primers) - Differerentiate through
- Sequencing
- Restriction endonuclease
- Single strand conformation polymorphism
35Presence absence of amplicon
- AAAGGGTTTCCCNNNNNNNNN
- CCCGGGTTTAAANNNNNNNNN
AAAGGGTTTCCC (primer)
36Presence absence of amplicon
- AAAGGGTTTCCCNNNNNNNNN
- CCCGGGTTTAAANNNNNNNNN
AAAGGGTTTCCC (primer)
37RAPDS use short primers but not too short
- Need to scan the genome
- Need to be readable
- 10mers do the job (unfortunately annealing
temperature is pretty low and a lot of priming
errors cause variability in data)
38RAPDS use short primers but not too short
- Need to scan the genome
- Need to be readable
- 10mers do the job (unfortunately annealing
temperature is pretty low and a lot of priming
errors cause variability in data)
39RAPDS can also be obtained with Arbitrary Primed
PCR
- Use longer primers
- Use less stringent annealing conditions
- Less variability in results
40Result series of bands that are present or
absent (1/0)