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Stem Cells Week 3 Lecture Notes

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June 20, 2023
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ACTIVE DNA METHYLAITON
(ARTICLE)

DNA methylation occurs
 DNA methylation has been observed during specific stages of development. predominantly in the
 DNA methylation process may be achieved by different enzymes and context of CpG (C
mechanisms. followed by G)
 The presence or absence of specific epigenetic marks influences gene dinucleotides.
expression, resulting in a transcriptional programme that specifies for a
particular cell type.
 In embryonic stem cells, active gene expression marks are found at
pluripotent genes and repressive marks are found at lineage-specific genes. During early development,
Thus, different cell types can be defined by their epigenetic and gene methylation patterns are
expression. initially established by the de
 The diversity of genetic material to be regulated necessitates the use of novo DNA methyltransferases
marks corresponding to short-term and ling-term epigenetic memory, DNMT3A and DNMT3B.
depending on the transcriptional requirements of the cell (as well as hose of
future generations).
 Developmental genes that are needed during the later stages of development are transiently held
in a repressed state during early development. This is achieved through short-term epigenetic
marks such as histone modifications, which can be removed before or within a few cell divisions.


* Active DNA Demethylation is the enzyme process that results in the removal of the methyl
group from 5-methylcytosine (5meC) by breaking a carbon-carbon bond.
* Passive DNA Demethylation refers to the loss of the methyl group from 5meC WHEN
DNMT1 is inhibited or absent during successive rounds of DNA replication.




METHYLATION DURING EARLY DEVELOPMENT


o Activation of different transcription factors during
gastrulation produces a single cell (zygote) to become all
cells in our body.
o Some genes that are expressed early on into gastrulation
can be switched of after a couple of developmental events
(e.g. the gene is switched on in 1-cell state and closes
during 4-cell state).
o If something goes wrong with the gene transcription, we
will see birth defects.
o In earlier days, pregnant woman would be treated
with thalidomide for morning sickness. Thus,
babies with birth defects on limbs were born.


DNA Elements
- All protein coding genes in the nuclear human
genome are transcribed by RNA polymerase II.

, - RNA polymerase II initiates transcription in conjunction with transcription factors.
- The expression of genes is determined by:
- The availability of transcription factors.
- The accessibility of the DNA element
(promoters/enhancers) to which
transcription factors bind (Methylation
of DNA, Histone modification)

- CpG dinucleotides often cluster in promoter areas.
- Methylated DNA can prevent transcription factors
binding.
- Methylated DNA can recruit proteins which
deacetylate histones.


Regulation of Methylation Marks
* Cytosine residues are methylated
* Regulation of transcription
* Regulation on X-inactivation
* Genomic imprinting



Removal of 5hmC, 5fC, or 5caC through:
1. Replication (active modification, passive dilution (AM-PD)); DNMT1 less efficient at methylating non
5mC strands.
2. Through thymine DNA glycosylase (TDG)/Base
Excision Repair (BER), (Active Modification).
Cooperation of TDG and BER leads to excision of
5fC/5caC and repair to C.
Genomic context-histone
acetylation makes DNA more
accessible to transcription
factors.

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