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Download Stem Cells from Skin Cells?!?
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Transcript
All cells in a person have the same DNA Yet eye cells differ from nose cells Central dogma of biology Genetic engineeri ng DN RNA A Niche factors Tissue therapy Protein Cell type Matrix Molecules Self-Renewal Soluble Factors Other Cells Differentiation Little, et al. Chemical Reviews (2008). Low stress levels Regular exercise Enriching experiences Learning new information Healthy diets: rich in antioxidants Avoid excessive drinking Skin cells iPS cells Are fully differentiated cells Can not become any other cell type Can only divide to make more fibroblasts Contact inhibition Randomly inserts DNA into genome of cells Can make special retroviruses with whatever gene you want Can’t really control how many copies of genes Only turn on a drug resistance gene when stem cell state Do this by using a gene that is only expressed in stem cells Add drug resistance to promoter region of that gene Takes around 16 days for resistance gene to be expressed- some secondary change Sox2- Self Renewal Oct4- Differentiation switch Klf4- p53 pathway, Oncogene c-Myc- Global Histone Acetylation, Oncogene Without Oct 3/4 or Klf: no colonies Without Sox2: rough morphology Without c-Myc: flatter cells, now know actually can do without c-myc-just very low efficiency Tried to inject into blastocyst to make baby mice but failed Final and best test of pluripotency Still working with mouse model Used different drug selection marker Same 4 genes Much more closely resemble ES cells Treatment of DNA with bisulfite converts cytosine residues to uracil, but leaves 5-methylcytosine residues unaffected Introduces specific changes in the DNA sequence that depend on the methylation status of individual cytosine residues Used Oct3/4, Sox2, Nanog and Lin28 Used the animal’s own cells- no immune rejection! Transfected with all four genes, but cmyc taken out after time- prevent tumors! Sickle Cell Anemia has known genetic basis-so target that gene and change it back to normal! Inject it back into the animal after radiation to reconstitute the whole blood system! Any disease with a single genetic mutation could be easily cured! Tissue regeneration after accidents or diseases “Nanobots” Companies have already started testing iPS for therapy No way FDA will approve a therapy with an oncogene Use of retroviruses can lead to mutations and cancers So many changes in the DNA can be harmful Probably hard to target to some areas
