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GENES & GENOMES > ROJW - cellular reprogramming > Flashcards

ROJW - cellular reprogramming Flashcards

1
Q

Cellular programming by nuclear transplantation

A
  • First performed by John Gurdon on a frog
  • Replace the nucleus of an egg cell with the nucleus from a differentiated somatic cell (ex. intestinal cell)
  • Can still result in development of a whole animal (information from the nucleus programs the development of the egg cell)
  • Proves that the nuclei of all cells harbor all the genetic materials required for the development of a whole animal
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2
Q

General principles:

A
  • All fully differentiated somatic cells contain a complete genome that is the same as the genome found in embryonic cells
  • But fully differentiated cells just express a subset of genes specific for a particular cell type that is different from another cell type (ex: a neuron vs. a hepatocyte – express different subsets of genes)
  • The different gene expression in different somatic cells are created and maintained by the expression of gene-specific transcription factors to establish and maintain tissue identity
  • Artificial nuclear reprogramming methods work by changing the expression of gene-specific transcription factors (thus change the subset of expressed genes) to change the cell type, or reset it to less differentiated stem cell states
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3
Q
  1. Totipotent stem cell
A
  • The early stage of fertilized egg cell
  • The most versatile stem cell type, because they are formed shortly after fertilization of an egg cell by a sperm cell
  • Can become all of the cells of the human body, as well as the cells of the embryo and developing fetus.
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4
Q
  1. Pluripotent stem cell
A
  • Can give rise to all of the cell types that form the human body, but are not as versatile as totipotent cells.
  • Can’t give rise to extra embryonic tissue that are required for embryogenesis
  • Differentiate into cells from any of the 3 germ layers
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5
Q
  1. Multipotent stem cell
A
  • Differentiate into a limited range of cell types which are more specialized/ specific
  • Involved in producing cells that are continuously produced in the body (ex. Blood cells)
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6
Q
  1. Final/ Fully differentiated cells
A
  • Committed to the function of the cell type that it has become to ensure tissue integrity
  • So usually, differentiation is not reversible
  • BUT: Somatic cells can be experimentally induced to change their identity by expressing one or more specific gene-specific transcription factors (artificially induced nuclear reprogramming)
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7
Q

Artificially induced nuclear reprogramming

A
  • Discovered in 2006 by Shinya Yamanaka
  • Expression of a combination of 4 gene-specific transcription factors: OCT4, KLF4, SOX2, and MYC (Yamanaka factors) - in any differentiated cells will revert it back to a pluripotent stem cell (forming induced pluripotent stem cells – iPSCs) that can differentiate into a variety of any other cell type – complete reprogramming
    o All these transcription factors, especially MYC, are also oncoproteins! overexpression and/or mutations in these proteins can be found in many types of human cancer
  • Possible therapeutic advantage to correct a problematic cell type (ex. neurodegenerative disease)
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8
Q

Anti-aging research can also use:

A
  • Partial reprogramming involves applying Yamanaka factors to cells for long enough to roll back cellular aging and repair tissues but without returning to pluripotency
  • Partial reprogramming can dramatically reverse age-related phenotypes in the eye, muscle and other tissues in cultured mammalian cells and rodent models by countering epigenetic changes associated with aging
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9
Q

Ex of Yamanaka factors:

A

OCT4

  • a moderately sized gene-specific transcription factor of (360 amino acids)
  • Has a “POU” DNA-binding domain is located centrally
    o consists of two helix-turn-helix motifs linked to each other
  • Transcriptional activation domains (ADs) located in the flanking N- & C-terminal portions
  • needs to be expressed in pluripotent cells to maintain their undifferentiated state
  • OCT4 acts with SOX2 to recognise and bind in a sequence-specific manner to DNA target sites located next to regulatory elements, driving the transcription of embryonic stem cell-specific transcription factors
  • Overexpression of OCT4 & SOX2 enforces aberrant the transcription of embryonic stem cell-specific transcription factors in differentiated cells, transforming them into iPSC
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10
Q

iPSC Characteristics

A
  • Immortal - no limit to number of cellular divisions (propagate indefinitely in cell culture)
  • Can be differentiated into any cell type found in the human body
  • Have a specific morphology
    o large prominent nuclei
    o narrow cytoplasm
    o defined border
    o tight cellular packaging
  • Express various specific proteins that are not expressed in differentiated cells (serve as pluripotency markers)
    o gene-specific transcription factors, such as OCT4
    o cell surface proteins, such as SSEA3, SSEA4,TRA-1-60, TRA-1-81
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11
Q

Applications of iPSC

A
  • Therapeutic cure of degenerative diseases (Stem cell therapy)
  • Genome edited iPSCs to cure genetic diseases
  • Experimental purposes
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12
Q

Therapeutic cure of degenerative diseases (Stem cell therapy)

A
  • Harvest cells from patients’ easily accessible tissues (ex. blood cells/ skin fibroblasts)
  • Grow in tissue culture
  • Introduce cloning vectors to overexpress Yamanaka factors – by virus/plasmids/mRNA to obtain iPSC
  • Differentiate the iPSCs to different cell types ex. pancreatic cells, cardiomyocytes, motor neurons – the cells that lacking in degenerative disease patients – and re-introduce them back to the right place
  • Create cells that are re-introduced into patients to cure/ reduce the severity of the diseases
  • Re-introduced iPSCs are genetically identical to the patients so there won’t be problems with immune rejection
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13
Q

Genome edited iPSCs to cure genetic diseases

A
  • In case of genetic disease, iPSC genome can be modified and corrected for any defects (ex. Knockout a gene that shouldn’t be on, add gene that is missing in the genome, correct mistake in the sequence of a gene)
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14
Q

Experimental purposes

A
  • Differentiate iPSC for desired cell types that are difficult get hold of
  • Ex. Cardiomyocytes, Neurons – and use them for drug screening purposes, mobile system for disease detection, especially genetic diseases – ex. Alzheimer’s
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15
Q

Differentiation of iPSCs

A
  • After obtaining iPSC from differentiated cells, the iPSCs need to be exposed to different growth factors at different stages to guide them through the differentiation pathway to produce the desired fully differentiated cell
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16
Q

Ex: Differentiation of iPSCs into Red Blood Cells

A
  • Laboratory techniques have been developed successfully to generate red blood cells (erythrocytes) from human iPSCs
  • could become an alternative treatment option for patients with blood disorders
  • sickle cell anaemia
  • various forms of a- and b- thalassaemia
17
Q

Pluripotency and Cancer

A
  • Several lines of evidence suggest that reprogramming to pluripotency and oncogenic transformation are related at the molecular and cellular level:
    o both processes induce a switch from an oxidative to a glycolytic metabolic state to generate E from glucose (don’t go through TCA cycle, does not require O2)
     cancer cells: before vasculated, do not have enough access to O2
     embryonic cell: early embryo has not differentiated heart and blood vessels, so low access to O2 too
    o both involve numerous chromatin factors and RNA binding proteins that cooperate with reprogramming factors
    o both lose cellular identity& acquire cell plasticity (rate-limiting steps for both reprogramming towards pluripotency and transformation into cancer cells)
18
Q

Cancer and Pluripotency has the same early steps

A
  • both require specific TFs to transform the cell to an intermediate cell type which characterize a high plasticity state (lose tissue-specific gene expression program)
  • cells then decide whether to develop into pluripotent or cancer cells (different paths)
19
Q

Problems with iPSC: Mutations

A
  • Some iPSC lines are heavily mutagenized, with a mutational burden similar to what is typically observed in human cancers
  • Mutations can be Due to 2 diff conditions:
    o Mutations present in original somatic cells used for nuclear reprogramming
     Cells that have existed for a long time could have acquired mutations that do not affect the function but no longer a WT genome – if get iPSC, will pass down mutations to iPSC
    o Mutations caused by cell culturing and in vitro reprogramming procedure
20
Q

Mutations Already Present in Somatic Cells

A
  • Usually, fibroblasts from skin cell samples are used for converting them into induced pluripotent cells (main reason: sampling from skin is easy)
  • iPSCs derived from such fibroblasts frequently contain a larger number of mutations than those derived from other cell types (due to exposure to sunlight thus UV radiation)
  • Any differentiated cells derived from such iPSC cell lines will also contain all these mutations, which increases the cancer risk for therapeutic applications
  • Therefore, using easily accessible cells like fibroblast runs a risk of having UV induced mutations ending up in the iPSC and increases the cancer risk for therapeutic applications
21
Q

Cell Culture-Induced Mutations

A
  • Culturing iPSCs in vitro causes additional mutations due to oxidative damage.
  • most frequently observed mutation in blood cell-derived iPSCs = single-nucleotide variants in gene-specific transcription factor BCOR (acts as transcriptional repressor)
    o BCOR is BCL6 corepressor, a key transcription factor identified as a potent oncoprotein in the lymphoid lineage
    o BCOR mutations are highly recurrent and oncogenic in mature T-cell lymphoma
    o Therefore, BCOR mutations that arise in iPSCs after reprogramming, can affect the global transcriptomic program of iPSCs and impede differentiation into neural lineages
  • BCOR can be statistically classified as a driver gene — a gene in which the prevalence of mutations is higher than would be expected by chance
22
Q

Practical, Social, Ethical and Legal Considerations

A
  • Consent of donor
  • Intellectual property and legal considerations (using other ppl’s cells – they might claim to have intellectual property rights)
  • Predisposition of recipients to cancer development (mutations already present in the somatic donor cells or caused during the reprogramming procedure may predispose cells to developing cancer when transplanted back into the patient)
    o Therefore, need:
     Informed consent
     High degree of protocols to ensure that reprogramming and cell differentiation is done in a safe environment
     Early detection of damaged cells

GENES & GENOMES (25 decks)

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