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Y3 (2) Epigenetics in Development and Disease > Lecture 8 - Weaver paper > Flashcards

Lecture 8 - Weaver paper Flashcards

1
Q

What is the background of the Weaver paper?

A
  • concerns the mechanisms whereby maternal effects or other forms of environmental programming are sustained over the lifespan of an animal
  • Previously known:
    • behaviour of mothers: licking, grooming, arched back attentive (high/low)
      • High LG-ABN - offspring less fearful, most HPA responses
      • Low LG-ABN - offspring more fearful, increased HPA responses
    • different offspring have different levels of GR
      • glutocortocoid is produced via the Hypothalamic-pituitary-adrenal (HPA) axis
    • tactile stimulation acts by serotonin
      • offspring of high LG-ABN mothers have enhaced GR expression that persists into adulthood
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2
Q

What is the Hypothalamic-pituitary-adrenal (HPA) axis? How does this related to the background of the Weaver study?

A
  1. Stress releases hypothalamic corticotropin-releasing factor (CRF)
  2. CRF acts on the pituitary-adrenal system
  3. This then releases glucocorticoid (steriod hormone - has lots of different activities in the organism)
  4. Elevated levels of GR (glutocortocoid receptor) enhances glucocorticoid negative feedback, resulting in a dampening down of this response

Already knew that the LG-ABN and HG-ABN animals have differnt levels of GR

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3
Q

Where releases glutocortocoid receptor?

A
  • Glutocortocoid is released from the adrenal gland
  • GR are found on the vast majority of mammalian cells
  • This study looked in the hypothalamus
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4
Q

How is tactile stimulation though to act on GR expression?

A
  • Acts via serotonnin
  • Tactile stimulation activates the serotonin pathway
  • Results in the activation of NGF1-A (TF) which binds to the binding site in the GR gene resulting in higher levels of GR
  • offspring of high LG-ABN mothers have enhanced GR expression that persists into adult hood
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5
Q

What was the aim of the Weaver paper?

A

How is the high expression of high LG-ABN maintained throughout life

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6
Q

What did the first figure (Fig 1a.) demonstrate and how was this acheived experimentall?

A
  • Knew: use of the GR gene 17 promoter is increased in offspring of high LG-ABN mothers (where NGF-1 TF binds)
  • Sodium bisulfite analysis of cytosine methylation status of the exon 17 GR promoter in adult offspring
    • looked at % methylation of these sites
    • offspring of low LG-ABN mothers have a higher % of methylation
  • Looked at the NGF1 binding site, 5’ and 3’ positions
    • big difference in C methylation in low LG-ABN (high methylation) compare to high LG-ABN (low methlation) in 5’ site but not 3’ site

Presentation of Data: 5 of methylation at each site

  • extract DNA -> PCR region of interest -> cloned individual PCR strands -> into plasmid vector -> sequence
  • Individual strands become % at each site
  • lose a bit of information
    • ​doesn’t make it clear whether at these sites they were 100% methylated or 0% methylation because all has been grouped together
    • instead use filled circle visualisation
    • shows some strands may be completely methylated/not at all
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7
Q

What did Fig 1d. demonstrate and how was this acheived experimentally?

A
  • Identified the behaviour of the mothers then switched offspring
  • the effect of cross-fostering the offspring of low and high LG-ABN mothers on cytosine methylation at the 5’ and 3’ CpG dinucleotides
    • cross-fostering occured within 12 hours of birth
  • Significance of this experiment: Is it the behaviour that is important. Does it take on the methylation due to the behaviour of the mother rather than a genetic factor
  • Get a profile of the foster mother not the birth mother
  • Results: same at 3’, at 5’ L-L and H-L have high CpG methylation, H-H and L-H have low CpG methylation
    • the behaviour of the mothers influences the methyaltion status
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8
Q

What did Fig 1e. demonstrate and how was this acheived experimentally?

A
  • Looked at the timing of the maternal effect on DNA methylation
  • the maternal care of low vs. high mothers differs only in the first week of life
  • post-natal changes in DNA methylation (aside from aging and cancer) were previously thought to be rare
  • Did time series
    • E20 before birth
    • P - days after birth (1, 6, 21, 90)
  • Results:
    • E20 - low methylation for low and high
    • By p1 - methylation for both becomes high (stress of birth?)
    • rapid drop in methylation post birth, in High LG-ABN, this is maintained
    • Low LG-ABN stays high
    • 3’CpG dinucleotide stays high for both
  • Thought that the default is high methylation
    • low levels of GR, weak dampening down reponse
    • strong fight/flight response
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9
Q

What pathway is active post birth in high LG-ABN offspring to bring down the methylation of the 5’ CpG dinucleotide for NFG1-A?

A

Activation of the seretonin pathway results in demethylation of the NGF1-A 5’ binding site

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10
Q

How was it shown whether the maternal effect on DNA methylation correlates with increased histone acetylation (H3K9-AC) and/or increased interaction between NGF1-A and the promoter?

A
  • ChiP - looking at the in vivo interaction between TF and DNA
  • A) H3K9 is a strong active mark
  • B) binding of the TF
  • I: input of ChiP; A: Immunoprecipitation (Ab); N: negative control (IgG not expected to pull down

Higher levels of active histone mark in High LG-ABN as have lower levels of DNA methylation (assocatied with inc. histone acetylation)

  • IP see 2 X PCR for the GR exon and the b-actin promoter (positive control, expect this promoter to have acetylated histones but would expect the same between La dn H offspring)

Looking at the TF

  • Er-a: exon promoter, control for input, to check the specificity of the Ab and the process, expect not to bind NGF TF
  • Bit in brackets - what being stained
  • See increased binding of the TF in high LG-ABN compared to low LG-ABN
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11
Q

How can the NG1 TF binding be linked with a change in histone acetylation?

A
  • already knew that NGF TF interacts with CBP (CREB binding protein (a histone acetyltransferase))
  • Activation of the TF recruit CBP to increase acetylation levels, resulting in more open chromatin, directing further and more stronger binding of NGF1

But why are the methyl groups removed?

  • 5hmC is a route by which get demethylation
  • or could be competition between open chromatin and ability of methyltranferase to act on this region
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12
Q

How was it shown whether the impact of these early experiences is reversible, and what was the result?

A
  • Histone deacetylase activity is inhibited by Trichostatin A (TSA)
    • pushing towards a more active confirmation
    • does this affect inhiition of transcription by DNA methylation?
      • MeCP2 binds region of methylated DNA and recruits the Sin3a co-repressor and a histone deacetylation, which recruits histone lysine methyltransferase to result in a change in chromatin stucture
  • When methylation is high (low LG-ABN) have low H3K9ac
  • When methylation is low (high LG-ABN) high high H3K9ac
  • Can this be shifted low to high?

Results - immunoprecipittion of Ab/input GR

  • Vehicle - need to dissolve trichostatin A in something, need to check the solvent isn’t having an effect
  • Look at acetylation levels and binding of TF in the vehicle in low LG and between the vehicle in high LG
    • Acteylation increases in the low LG-ABN and in the high LG-ABN but only to a significant level in the low LG-ABN
  • Look at level of NGF1-A to see if correlates
    • see same pattern
  • Also looked at DNA methylation as a result
    • DNA methylation decreased at 5’ site between vehicle and low LG-ABN significantly (not in high LG-ABN)
    • Also decreased in the 3’ site for both high and low LG-ABN
  • Looked at whole region
    • General reduction in methylation between the vehincle and treatment but not always significant
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13
Q

Why does TSA treatment result in loss of DNA methylation?

A
  • chromatin modifications are dynamic
  • balance between acetylation and methylation
  • If inhibit deacetylation it is pushed towards demethylation by an undefined mechanism
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14
Q

How was it shown whether GR levels are increased by TSA treatment?

A
  • Used western blot to look for GR levels
  • Antibodies to detect
    • GR
    • a tubulin (loading control - although TSAis a broad spectrum epigenetic drug so may have an effect)
  • Inreased levels of the receptor in high Lg-ABN not in low LG-ABN
  • with TSA get incresaes in both both not significant aside from in the low- LG-ABN
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15
Q

How was it demonstrated the effect of TSA treatment affecting HPA responses to stress?

A
  • Measured levels of stress by the steroid hormone corticosterone levels
  • Observed with and without TSA
  • Stress increased by restraining
  • Measured before, during and after restraint
  • Results:
    • In all animals see a dampening down effect
    • Before restraint, the low LG-ABN already had increased levels of the steroid hormone
      • similar profile to teh others in the timing of the dampening down
  • Looked at levels of GR alongside
    • high GR in low maternal
    • even with high GR still get a response (important in nature)
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16
Q

What were the implications of the weaver et all study?

A
  • Epigenome is suceptible post embryonic development
  • early life experiences can impact into adulthood
  • Some processes may remain sensitive to environmental regulation thoughout life
  • effects of early life experiences are reversible using drugs that target epigenetic modifications
  • potential for using epigenetic drugs to treat psychiatric disorders in humans
17
Q

What are the limitations and possible future work of the Weaver study?

A
  • this study was conducted before knowledge of 5hmC
  • bisulfite analysis won’t distinguish between 5mC and 5hmC
  • Instead use TAB-assited bisulfite sequncing
  • are the levels genuinely 5mC
  • 5hmC pathway involved in demthylation (as cells aren’t replicating must be an active methylation process)
  • Use other inhibitors e.g. DNA methylatransferase inhibitors
  • Instead of looking at a single region of the gene do the whole genome with TAB assisted bisulfite analysis to identify what other genes are changing
18
Q

Can the Weaver study be extrapolated into humans?

A
  • Later study had access to toronto brain bank
  • Looked at the human equivelent of this gene
  • Brains from:
    • people died in accidents
    • commited suicide
  • Had an idea of whether these people suffered early childhood abuse
  • Saw same pattern
  • significantly different methylation patterns

Future work could look at other tissue samples that are more accessible e.g. circulatory cells

Y3 (2) Epigenetics in Development and Disease (8 decks)

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