Aliens? Oddities? Or misunderstood? - PowerPoint PPT Presentation

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Aliens? Oddities? Or misunderstood?

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Aliens? Oddities? Or misunderstood? Transposons and miRNAs Genome sizes (haploid) Number of genes in different organisms What is a transposon? Contiguous piece of DNA ... – PowerPoint PPT presentation

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Title: Aliens? Oddities? Or misunderstood?


1
Aliens? Oddities? Or misunderstood?
  • Transposons and miRNAs

2
Genome sizes (haploid)
3
Number of genes in different organisms
4
What is a transposon?
  • Contiguous piece of DNA of varying length (300 bp
    to 6.5kb or so)
  • Repeated with minor variations throughout the
    host genome
  • Can replicate itself by cut and paste or copy and
    paste mechanisms (can move around!)
  • No known function most synthetic genome
    projects aim to remove them
  • Structural and functional analogies to viruses
  • Much of the terminology reflects this

5
  • Barbara McClintock, 1940s
  • Discovered transposons and characterized their
    effects on their hosts
  • She was ostracized for her ideas but won the
    Nobel Prize in 1983.

6
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7
Types of transposons
  • Cut and paste
  • DNA transposons
  • Copy and paste
  • Autonomous retrotransposons
  • ERVs possibly active in human genome
  • L1 relatives active in human genome
  • Nonautonomous retrotransposons
  • SINEs (Alu) active in human genome
  • SVA active in human genome
  • Composite element (SINE, VNTR, Alu)
  • Processed pseudogenes

8
Transposons comprise 45 of the human genome
  • DNA transposons 3
  • Autonomous retrotransposons
  • ERVs
  • L1 18 (500,000 copies)
  • L2 3
  • L3 relatives 1
  • Nonautonomous retrotransposons
  • SINEs (Alu) 15 (1 million copies)
  • SVA (3000 copies)
  • Processed pseudogenes (gt8000)
  • (Simple repeats occupy almost another 10)


LTR retrotransposons
9
Junk DNA?
  • What do transposons do?
  • Make more of themselves
  • Move genes around
  • Serve as reservoirs of new sequence
  • Cause genetic instability (repeats stimulate
    translocation L1 causes chromosome breakage)
  • Can contribute to genes and gene expression
  • 5 of alternatively spliced internal human exons
    come from Alus
  • 80 of genes have some L1 sequence in noncoding
    portion
  • 1-4 of coding sequence is L1-derived
  • Act as methylation centers

10
Importance in genomics
  • Transposons are a source of human variability
  • Roughly 5 of people have a transposon not found
    in either parent (not due to nonpaternity!)
  • Overall polymorphism variable but remarkable
    (40-50 of youngest elements are polymorphic)
  • Transposons can be useful in medicine
  • Occasionally cause disease (de novo insertion in
    factor VIII clotting gene led to L1 discovery in
    1980s)
  • May often be linked to disease loci

11
Importance in genomics
  • Transposons in introns may disrupt gene
    expression
  • Mechanism depends on whether they are on the
    sense or antisense strand
  • () strand orientation transcription stalling
  • (-) strand orientation premature
    polyadenylation, gene splitting

12
Importance in genomics
  • Can have huge effects, through chromosomal
    translocation, inversion, breakage

13
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14
Transposon domestication
  • Overly active transposons will kill a cell (and
    then the organism)
  • Transposons have tempered
  • active almost exclusively in germ line
  • also in cancer cells and neuronal cell precursors

15
Transposon domestication
  • Host cells use many mechanisms to control
    transposons
  • Methylation (original role?)
  • miRNA defense
  • Sequestered in stress granules
  • Nucleic acid editing
  • APOBEC family of proteins edits cytosines to
    uracils
  • ADARs edit dsRNA adenosine to inosine

16
What to do with transposons?
  • Study them
  • Work around them (be aware)
  • RepeatMasker (Smit Jurka)
  • Problem each element is at least in part unique,
    and RepeatMasker will mask that too

17
Another old element, new to sciencemicroRNAs
  • RNA world hypothesis
  • First organism was a strand of RNA that could
    somehow replicate itself.
  • Eventually RNA used DNA as a more stable storage
    for genetic material.
  • 1982 Tom Cech reported self-splicing RNAs

18
microRNA
  • 21-25 nucleotide small RNAs
  • Discovered in a C. elegans screen
  • Alter gene expression at the post-transcriptional
    level (precise mechanism unknown)
  • Tend to be high-level regulators (gt100 targets
    each)
  • Percentage of human genes under miRNA control is
    unknown but possibly 20-30
  • Often are developmental or cell state switches

19
miRNA
20
Two mechanisms Perfect match to target leads to
mRNA cleavage or Imperfect match leads to
translational repression Neither is
well-understood, but likely involve the dsRNA
recognition system
21
Another role?
  • Under conditions of cell stress, a miRNA may be
    activating instead, as responding regulatory
    proteins interpret the signal differently

22
Seems odd . . .
  • Why would a cell use this sort of mechanism? Its
    making an mRNA and then degrading it. Should be
    easier to just not make it . . .
  • But what if the cell is not in control of that
    RNA, for example if its coming from an invasive
    nucleic acid species under its own promoter?
  • Transposon control!!!
  • piRNA (piwi RNA) are a whole class of small RNAs
    that control transposons
  • Invasive RNA was a big problem in the RNA world!

23
Occams razor
  • All other things being equal, the simplest
    solution is the best
  • My alternative If a biological principle is
    simple, its probably wrong.
  • Evolution tends to higher complexity, as old
    mechanisms are reused and theres little
    incentive to clean up.

24
Looking for new miRNAs
  • Often found within stem-loop precursor structures
    (hairpins)
  • Associated (in the cell) with polysomes and other
    structures
  • Bioinformatics unexpected sequence conservation
    in noncoding region, or homology to miRNA in a
    closely related species (works less often than
    you would think)
  • Identify candidate miRNA targets (TargetScan, by
    Chris Burges group)
  • A target protein usually has multiple target sites

25
Problems with miRNAs
  • Small! Unstable, hard to get large quantities
  • Binding is degenerate, noncontiguous, and
    includes not only mismatches but bulges
  • Actual sequence recognition only 15 or so
    nucleotides (noncontiguous), varies by target
  • Essential seed element not well characterized
  • Sequences not well conserved across species
  • miRNA microarrays statistics problematic because
    there are so few spots
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