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Our DNA is what makes us who we are. It determines our hair texture, skin colour, eye colour, and everything else within our bodies. Would you be surprised if you knew that our DNA can change? Changes in the physical structure of our DNA are attributed to epigenetics. Epigenetics also play an important role during development and are responsible for regulating stem cells to form the vast amount of cell types that make up our body. Each cell has the same DNA sequence, so we need epigenetic regulation (changes to the accessibility of the DNA for transcription) to allow different expression patterns in each type of cell, which are the cause for the specialization and differentiation of each cell type.
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Jetzt kostenlos anmeldenOur DNA is what makes us who we are. It determines our hair texture, skin colour, eye colour, and everything else within our bodies. Would you be surprised if you knew that our DNA can change? Changes in the physical structure of our DNA are attributed to epigenetics. Epigenetics also play an important role during development and are responsible for regulating stem cells to form the vast amount of cell types that make up our body. Each cell has the same DNA sequence, so we need epigenetic regulation (changes to the accessibility of the DNA for transcription) to allow different expression patterns in each type of cell, which are the cause for the specialization and differentiation of each cell type.
During fetal development, stem cells are capable of extensive self-renewal and can differentiate into many cells. For a stem cell to commit to one lineage, long-lasting changes in gene expression must be made to prevent these stem cells from self-dividing into more stem cells. This is done through epigenetic changes. Epigenetic mechanisms such as DNA methylation and histone modification are vital for controlling stem cell differentiation during development.
A stem cell lineage is a group of differentiated cells that all come from the same stem cell. Depending on the epigenetic changes that happen to a particular stem cell, in the embryonic or adult stage of development, that stem cell could differentiate into a certain group of cells. For example, it might become a hematopoietic stem cell, which can only generate blood cells.
Stem cells have two essential properties: the ability to self-divide and the ability to differentiate into many cell lineages. A single embryonic stem cell can divide into more stem cells and these can differentiate into any specific cell within the body. For example, a stem cell can turn into a skin cell, a cardiomyocyte, or even a natural killer cell depending on the epigenetic changes that it goes through.
What organ is home to cardiomyocytes?
Epigenetic regulation controls access to the DNA before DNA transcription is initiated. The primary epigenetic mechanisms that we will be discussing in this article are: DNA cytosine methylation and histone modification. Let's take a closer look at both these mechanisms.
Epigenetic regulation refers to the biological processes that regulate heritable changes in gene expression without changing our DNA sequences.
As DNA is organized within a chromosome, it is wounded around strands of histone proteins.1 These histone proteins package the DNA into structural units called nucleosome complexes, which are responsible for regulating which enzymes have access to certain DNA regions.1
Histones are specialized proteins that bind to DNA and wrap DNA around them. This wrapping hides genes from the transcription machinery which prevents these genes from being transcribed. Recall that all cells have the same exact genetic code; however, each type of cell has a different expression of this genetic code. Some cells have certain genes expressed that another cell may not. Variations in gene expression are what create unique cell types.
If a specific gene needs to be transcribed, the nucleosome surrounding the DNA region carrying the gene can slide down the DNA to give the transcriptional machinery access to that given region.
Think of a roll of toilet paper. You cannot see each square within the roll because it is rolled up. If you wanted to use the 20th square because a gene is there that needs to be transcribed, you would have to unroll the toilet paper in order to find the 20th square.
Nucleosomes uncover DNA segments by unrolling the specific DNA segment with the gene that needs to be expressed. Nucleosomes can move to expose a segment of DNA; however, they do so in an extremely controlled manner. When nucleosomes are close to one another, they cover up a large segment of DNA, and the genes within that segment cannot be expressed since the transcriptional machinery cannot access them.
The way histone molecules (the components of the nucleosome) move to expose DNA segments is dependent on signals found both on the histone proteins and on the DNA.1 These signals are special tags that are added to the histone and the DNA that tell the histones if a chromosomal segment should be exposed or not. The special tags can be added or deleted as needed based on which genes need to be transcribed. A tag can be phosphate, methyl, or acetyl groups that attach to amino acids within the histone protein or to nucleotides within DNA. These tags alter how tightly wound the DNA is around the histone protein.1
What charge does an acetyl group have?
DNA has a negative charge which means that changes in the charge of the histone will change how tightly wound the DNA molecule will be. Without the tags, histone proteins are positive which attracts the negative DNA resulting in a tightly wound nucleosome. When tags like phosphate groups are added to the histone protein, it becomes negatively charged which repels the DNA molecule resulting in a loosely wound nucleosome.1
DNA methylation is the addition of a methyl (-CH3) group to the DNA strand at the 5th carbon atom of a cytosine ring.1 Once the methyl group attaches to the 5th cytosine carbon, they create 5-methylcytosine which is catalyzed by enzymes called DNA methyltransferases (DNMTs).1
In mammals, DNA methylation occurs mainly at the CpG dinucleotides which are stretches of DNA with a high number of cytosine and guanine dinucleotide pairs.1 At these CpG dinucleotides, DNMTs called DNMT3a and DNMT3b establish methylation patterns by working together to create de novo methylation. On the other hand, methylation has to also be maintained: there also exist maintenance DNMTs, which copy the established methylation patterns onto newly replicated DNA strands.1
Can you recall the base pairing rule?
DNA methylation changes how DNA interacts with histone proteins. Highly methylated DNA regions are tightly coiled and do not participate in transcription.1 Epigenetic changes to DNA and histones do not alter the codons within the DNA so each DNA codon remains intact. Also, epigenetic changes are not permanent. Instead, they simply control which segment of DNA can be transcribed. A gene can be turned on or off depending on the epigenetic modifications discussed above.1
A wide array of RNA classes ranging from small RNAs to long non-coding RNAs have been identified as key regulators of gene expression.4 From the previous section, we understand that histone modification and DNA methylation drive the regulation of gene expression by controlling what genes are transcribed. Small RNAs control gene expression by recruiting epigenetic factors such as the ones mentioned above. The RNAi pathway is the primary pathway for RNA-mediated epigenetic regulation of stem cells.4 RNAi is a group of mechanisms that utilize small RNA molecules to facilitate gene silencing.4
We know from the regulation of gene expression article that most eukaryotic genes are transcribed by RNA polymerase II. Once transcribed, the RNA transcript is spliced and then exported into the cell's cytoplasm.4 Within the cytoplasm, ribosomes catalyze the translation of RNA into proteins.4 During this process, small RNA molecules are able to exert their silencing effects.
During translation, mRNA sequences are converted into protein amino acid sequences. During translation, tRNAs bring the necessary base pairs to form the amino acid codons while ribosomes assemble these codons into an amino acid sequence.
There are many types of regulatory small RNAs, including small interfering RNAs (siRNAs) and micro RNAs.4 The double-stranded precursors of siRNAs and microRNAs bind to Dicer, which is an endonuclease protein that cuts RNA into short segments.4 These segments can then bind to an Argonaute protein where they are unwoven and a single strand remains bound to Argonaute.4 The single-stranded segment along with the Argonaute protein form the RNA-induced silencing complex (RISC). siRNAs tell RISC to bind to certain mRNA transcripts within the cytoplasm.4 The siRNA segment bound to the Argonaute protein can only bind to mRNA that is complementary to the siRNA segment.4 Once the RISC complex is bound, the Argonaute protein cleaves the mRNA transcript and the rest of the transcript is degraded causing the transcribed gene to be silenced.4
Argonaute proteins: Specialized proteins that play key roles in stem cell regulation and RNA silencing.
Epigenetics play a crucial role in cell differentiation by regulating which genes are expressed. The regulation of gene expression determines the cell lineage that a stem cell divides into. Stem cells are capable of asymmetrical cell division, which means that they can divide into two different types of cells. In other words, a multipotent stem cell can divide to create two daughter cells with different lineages: for example, one can be a neural precursor cell and the other a muscle precursor cell.
Can you recall the epigenetic factors that condition a cell's lineage discussed above?
As a cell receives a signal, genes within that differentiating cell turn on and drive that cell toward a specific lineage. If a stem cell receives a signal telling it to differentiate into a nervous system cell, this stem cell will only express genes needed to form a nervous system cell. Another way that cell differentiation can be controlled is through environmental stimuli.
An example of this phenomenon can be explained using the heat shock factor protein. If a cell is exposed to too high a temperature, the heat shock factor will migrate into the nucleus and influence the cell's gene expression to create more heat shock proteins within the cell. These heat shock proteins will then form a hardened barrier around the cell to protect it from the high temperature. Cells within our body also produce heat shock factors in response to low oxygen.
Now let's look at a specific example of how a cell responds to internal, external, and environmental signals to establish cell specialization.
The adult brain has two main regions where neurogenesis occurs: the subventricular zone (SVZ) and the dentate gyrus, located in the hippocampus. Within the SVZ, astrocytic stem cells differentiate into early neurons, called neuroblasts, and glial cells. When an astrocytic stem cell divides, it can produce either a neuroblast, transient amplifying cell, or another astrocytic stem cell in any combination. If the astrocytic stem cell divides into a neuroblast, a neuron will be produced.
Can you recall the types of glial cells?
Once the neuron is produced, internal and external signals will drive it toward a specific specialization. In the case of the subventricular zone, the neuron will be an olfactory neuron that specializes in transmitting chemical stimuli to the brain. On the other hand, if the astrocytic stem cell divides into a transient amplifying cell, a glial cell will be produced. Specific signals will drive that cell to either produce an astrocyte or an oligodendrocyte.
The level of specificity of a differentiating cell depends on which internal and external signals are present, as well as the location of the cell. The cell's location and signal stimuli determine what transcription factors are activated, which will determine what genes are expressed in that particular cell. A cell's gene expression is what determines its specialization.
Cancer is, simply put, uncontrolled cell division. Uncontrolled cell division may seem great at first since it could possibly lead to immortality; however, each new cell needs space and sustenance, causing a grievance to the other cells in the organism.
When a cancer cell divides, there is no control over what type of cell will be produced. For example, people with lung cancer can have teeth cells and bone cells develop in their lungs which hurts the lungs as blood flow interruptions and structural damage to the lungs can occur. The primary treatment for cancer is chemotherapy which is the introduction of harmful chemicals into the affected organism in an extremely controlled way in order to only kill the target cancer cells.
Transcription of oncogenes is the primary cause of cancer.
Chemotherapy is not effective in stopping all cancers which is why researchers are looking for new options. One of these treatment options is using epigenetics to regulate cancer cells. Researchers at the Northwestern University of Medicine discovered an epigenetic complex that works to allow widespread cell division in cancer cells.3 This complex is called the polycomb repressive complex 2 (PRC2).3
This complex is a methyltransferase like the ones we discussed above in the DNA methylation section.3 Usually, this complex is inhibited by DNA methylation. The methylated gene that inhibits PRC2 is called CATACOMB (Catalytic Antagonist of Polycomb). Usually, this gene is silenced in our genome due to DNA methylation.3 However, when the level of methylation is very low, the CATACOMB gene can be expressed and can bind to the PRC2 complex and inhibit its activity.3 This CATACOMB gene has the potential to utilize epigenetics to inhibit cancer cell activity and regulate cancer cells.3
As DNA is organized within a chromosome, it is wounded around strands of histone proteins. These histone proteins package the DNA into structural units called nucleosome complexes, which are responsible for regulating which enzymes have access to certain DNA regions.
DNA methylation is the addition of a methyl (CH3) group to the DNA strand at the 5th carbon atom of a cytosine ring.
Epigenetics play a major role in cell differentiation and cell specialization. Epigenetics function to regulate gene expression to control what genes are expressed in which cells. Controlling gene expression allows for a wide range of cells, each with different functions.
Epigenetic regulation is the control of gene expression through the modification of DNA. Epigenetics include histone modification and DNA methylation.
An example of epigenetic regulation is histone modification. Histones bind to DNA and roll up sections of genes so that they cannot be expressed.
Yes. Epigenetics regulate gene expression. Regulating gene expressions allow cells to differentiate into specific lineages.
Yes. Epigenetics regulate hematopoietic stem cell development by controlling the gene expression of precursor stem cells.
Flashcards in Epigenetic Regulation of Stem Cells15
Start learningAll cells control the synthesis of proteins via genes encoding in their DNA.
True
Why are stem cells important in biology?
They have the potential to self-renew
What are the two essential properties of stem cells?
The ability to self renew
What are embryonic stem cells?
Stem cells found during fetal development
Stem cells that are capable of differentiating into all body cells are called____.
Pluripotent
_____ refers to the biological processes that regulate heritable changes in gene expression without changing our DNA sequences.
Epigenetic regulation
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