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Stem cells

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Stem cells Helena Fulkova Institute of Animal Science fulkova.helena_at_vuzv.cz – PowerPoint PPT presentation

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Title: Stem cells


1
Stem cells
  • Helena Fulkova
  • Institute of Animal Science
  • fulkova.helena_at_vuzv.cz

2
Stem cells
  • Totipotent zygote (2-cell stage embryo)
  • Pluripotent embryonic stem cells
  • Multipotent (Unipotent) adult stem cells

3
Stem cells II
  • Division
  • - Asymmetric (1 stem cell 1 differentiated
    cell)
  • Symmetric (2 stem cells)

4
Stem cells III
  • From embryos ESC (embryonic), TSC
    (trophoblast), XEN cells ? (extraembryonic
    endoderm), Epi SC (epiblast - postimplantation)
  • Adult testicular, ovarial ???, tissue specific
    (skin, liver), mesenchymal (bone marrow, adipose
    tissue, peripheral blood )
  • iPS cells induced pluripotent stem cells

5
Embryonic stem cells
  • First differentiation blastocyst (ICM vs. TE)
  • Dependent upon Oct4 vs. Cdx2 expression

TE
ICM
6
Oct4
Cdx2
7
Nanog
DAPI
8
ESCs embryonic stem cells
  • Human, mouse, Rhesus monkey (rabbit, rat?)
  • From ICM cells
  • Expression
  • intacellular (Oct3/4 (Pou5f1), Nanog, Sox2 )
  • - cell surface (SSEA1 mo, SSEA4 hu,
    TRA-1-60 and TRA-1-81 hu)

9
Derivation and culture
  • Feeders vs. Feeder- free system
  • (MEFs, STOs, SNLs vs. Gelatin, Matrigel, 3T3
    cell matrix )

DAPI
SSEA1
10
Derivation and culture II
  • LIF (Leukemia inhibitory factor) Mo
  • BMP Mo
  • FGF Hu (LIF independent)
  • Activin (inhibin A) /Nodal - Hu
  • FCS (ES tested) or KOSR

11
Differentiation - pluripotency
  • The ability to differentiate into all three germ
    layers ectoderm, mesoderm, endoderm (in vitro
    and in vivo)
  • Lineage specific markers
  • Meso (muscles skeletal, cardiac, blood )
  • Ecto (skin, neuronal cells - CNS )
  • Endo (digestive tube derivatives)

12
In vitro differentiation
  • Mostly through EBs formation

13
In vivo not applicable to human!
  • Chimera production injection of ES cells into
    blastocysts
  • Teratoma formation injection of ESCs into
    immunodeficient mice (SCID)

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Advantages
  • In vitro manipulation, large quantities (tissue
    engineering, genetic manipulations, germ line
    transmission )
  • Excellent model for random X chromosome
    inactivation, general differentiation mechanism
  • Hope for cell (tissue) based therapy - Hu

16
Problems
  • Very sensitive cells fast differentiation
  • Unstable karyotype
  • XX lines (loss of one X chromosome)
  • - trisomy of chromosome 8
  • a BIG problem for possible therapy

17
Normal
Abnormal
18
Epigenetic properties of ESCs
  • Bivalent domains (H3K4, H3K27 methylation)
    promoters of tissue specific genes
  • Global hypomethylation
  • Chromatin loosely organised hyperdynamic
    (hyperplastic) chromatin (good donors for SCNT)
  • Both X chromosomes active

19
Epigenetic mechanism of differentiation
  • Stabilization of histone modifications in
    promoter regions
  • Methylation of promoters of pluripotency-associate
    d genes
  • Changes in genome organisation, random X
    chromosome inactivation
  • . Implication for SCNT and iPS technology

20
Li et al., 2007, Mol Cell Biol
Meshorer et al., 2006, Dev Cell
21
Possible application Therapeutic cloning cell
therapy
  • Somatic Cell Nuclear Transfer
  • Donor (any somatic cell from a patient)
  • Recipient (oocyte Hu or other specie ISNT)
  • No problem with tissue rejection!

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Disadvantages
  • Lack of human oocytes
  • SCNT does not work in humans (?)
  • ISNT poor compatibility of cytoplasm and
    nucleus (poor reprogramming, mtDNA, embryonic
    genome activation )

25
ISNT
26
ISNT II
B X B 96h
P x B 96h
27
Trophoblast stem cells - TSCs
  • Derived from TE (Cdx2, Eomes)
  • FGF4 heparin (MEF conditioned medium)
  • Chimeras only trophoblast lineage
  • Imprinted X-inactivation
  • Differentiation into giant cells

28
XEN cells Extra embryonic endoderm
  • True stem cells?
  • From ICM, on MEFs in TE culture media (RPMI
    FGF4, Heparin)
  • Chimeras only extra-embryonic endoderm lineages
  • Imprinted X-inactivation

29
Epiblast stem cells - EpiSCs
  • Mouse, Rat Activin/Nodal signalling (Human
    ES-like)
  • Postimplantation embryo epiblast
  • Oct4/Nanog/Sox2 expression
  • Monolayer morphology
  • Chimera no contribution
  • Teratomas - Yes

30
Induced Pluripotent Stem cells iPS cells
  • Possible application cell therapy
  • Induction of ES-like cells from cell cultures
  • Viral transduction or transfection

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Good laboratory practice
  • Cell culture
  • ESC characterization

34
Cell culture
  • Dedicated area restricted access
  • Keep a good record of lines (lines, clones)
  • Use cell culture tested reagents (ESC tested)
  • Mycoplasma testing

35
ESCs characterization
  • Karyotype (every 5th passage)
  • Markers of pluripotency (IF, RT PCR)
  • Differentiation (all 3 germ layers at least in
    vitro see NIH page for hESCs registry and rules
    for submitting a new line)

36
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