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ANAT3231: lectures overview Dr Annemiek Beverdam – School of Medical Sciences, UNSW Wallace Wurth Building Room 234 – [email protected] Stem Cell Biology Stem Cell Technology Resources: http://php.med.unsw.edu.au/cell biology/ Essential Cell Biology – 3 rd edition Alberts

ANAT3231: lectures overview - … lectures overview ... Stem Cell Biology Stem Cell Technology Resources: ... Dong et al., Nature 2014 Pluripotent stem cells

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Page 1: ANAT3231: lectures overview - … lectures overview ... Stem Cell Biology Stem Cell Technology Resources: ... Dong et al., Nature 2014 Pluripotent stem cells

ANAT3231: lectures overview

Dr Annemiek Beverdam – School of Medical Sciences, UNSW Wallace Wurth Building Room 234 – [email protected]

Stem Cell Biology

Stem Cell Technology

Resources: http://php.med.unsw.edu.au/cell biology/

Essential Cell Biology – 3rd edition Alberts

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ANAT3231: lab next week

Dr Annemiek Beverdam – School of Medical Sciences, UNSW Wallace Wurth Building Room 234 – [email protected]

Journal club presentation

Student groups

Choose 2-3 articles and send me PDFs by Friday afternoon 5 pm

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ANAT3231: lectures overview

Dr Annemiek Beverdam – School of Medical Sciences, UNSW Wallace Wurth Building Room 234 – [email protected]

Stem Cell Biology

Tissue homeostasis and regeneration Stem cell biology Stem cell niches

Stem cell regulation Stem cells and cancer

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ANAT3231: lectures overview

Dr Annemiek Beverdam – School of Medical Sciences, UNSW Wallace Wurth Building Room 234 – [email protected]

Stem Cell Technology

Regenerative Medicine Stem Cell Sources

Future of Regenerative Medicine Knock-out Technology

CRISPR/CAS9 Genome Editing

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Regenerative medicine the clinical application of stem cells

"process of replacing or regenerating human cells, tissues or organs

to restore or establish normal function"

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Stem Cell Sources for Regenerative Medicine

Multipotent

Stem cells derived from embryos

Stem cells derived from adults

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Stem Cell Sources for Regenerative Medicine Waddington's model of epigenetic determination of development

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Embryonal Carcinoma Cells are pluripotent

1964 – Pierce and Kleinsmith isolate EC cells from teratocarcinomas Source: gametes

Pluripotent In vitro culture and expansion

Genetic abnormalities

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Embryonic Stem Cells are pluripotent

1981 – Martin Evans, Matthew Kaufman and Gail Martin

Pluripotent No genetic abnormalities

In vitro culture and expansion Ethical issues

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Adult stem cells

“An undifferentiated cell, found among differentiated cells in a tissue or organ that can renew itself and can differentiate to yield some or all of

the major specialized cell types of the tissue or organ”

-  Bone marrow stem cells: haematopoietic stem cells -  Neural stem cells -  Intestinal stem cells -  Skin stem cells -  Umbilical cord stem cells: haematopoietic stem cells

No ethical issues Restricted plasticity Limited quantities Hard to identify

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Somatic Cell Nuclear Transfer John Gurdon, 1958

The developmental potential of nuclei of differentiated cells

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Somatic Cell Nuclear Transfer

“mature, differentiated cells can be reprogrammed to become pluripotent”

Pluripotent (totipotent?) Low success rate

Genetic/phenotypic abnormalities Ethical issues

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Reproductive/Therapeutic Cloning

Pluripotent (totipotent?) Low success rate

Genetic/phenotypic abnormalities Ethical issues

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Nuclear Reprogramming Induced pluripotency (iPS), Yamanaka, 2006

“mature, differentiated cells can be reprogrammed to become pluripotent”

Oct4 Sox2 c-Myc Klf4

2-3 weeks

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Nuclear Reprogramming Induced pluripotency (iPS), Yamanaka, 2006

“mature, differentiated cells can be reprogrammed to become pluripotent”

Oct4 Sox2 c-Myc Klf4

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Stimulus-Triggered Acquisition of Pluripotency (STAP) (Obokato 2014, controversial)

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Stem Cell Sources Embryonic vs Adult Stem Cells

iPS Cells

-  Can generate any cell type -  Easy to generate, maintain

and grow in lab -  Perfect genetic match to

patient

-  May retain age of parental cell

-  Inheritance of mutations: teratomas

-  May retain age of parental cell

-  Inheritance of mutations: teratomas

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The Future of Regenerative Medicine

! ?

?

?

?

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Future Stem Cell Technologies

1- how we can induce and maintain pluripotency? 2- how we can direct differentiation? 3- how we can cure diseased cells? 4- how we can repair mutations in cells?

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Future Stem Cell Technologies

How can we direct differentiation? -  Uncontrolled differentiation

-  Directed differentiation

? ?

?

? ?

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Future Stem Cell Technologies Directed differentiation of cardiomyocytes

Mummery et al., Circ Res 2012

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Future Stem Cell Technologies Directed differentiation of motor neurons

Dong et al., Nature 2014

Pluripotent stem cells

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Future Stem Cell Technologies Directed differentiation of pluripotent stem cells

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Future Stem Cell Technologies

How can we direct differentiation?

Directed differentiation: learn from developmental biology!

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Future Stem Cell Technologies

How can we cure disease?

Disease Modeling and Drug discovery

(personalized medicine)

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Future Stem Cell Technologies

How can we repair mutations in cells?

Gene Therapy:

Knock out technology

CRISPR/CAS9 genome editing

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Crossing over is a natural process that happens during meiosis

Knock out technology = directed homologous recombination in pluripotent ES cells

Knock out technology

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Endogenous gene

ATG

neoR

= regions of homologous DNA sequence

neoR

Targeting vector

Knock out allele

Homologous recombination

Knock out technology

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Knock out technology

1 Creating knockout DNA construct

3. Heterozygous mutant ES cells

2. Generating embryonic stem cells

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Chimeric mice

Genetic crosses to obtain Homozygous mutant mice

Heterozygous mutant Embryonic stem cells

Knock out technology

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Knock out technology Engineering of targeting vectors

Repair mutations

*

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Knock out technology Engineering of targeting vectors

Expressing multiple genes from same GM locus

Gene X

Gene X

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Knock out technology

Allows us to:

Study gene function in mice

Repair mutations or to express a second protein from a GM locus in ES cells

However:

Heterozygosity in recombined ES cells

(Low rates of homologous recombination)

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CRISPR/Cas9 Genome Engineering (Clustered Regularly Interspaced Short Palindromic Repeats)

Guide RNA and Cas9

http://www.youtube.com/watch?v=0dRT7slyGhs

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CRISPR/Cas9 Genome engineering Repair

Homology-directed repair: Provide donor template with homology arms

Gene mutation/correction/addition (Cas9 D10A mutant)

Non-homologous end joining: Small insertion/deletion

gene disruption (and occasional errors)

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CRISPR/Cas9 Genome engineering Applications in Stem Cells

ES cells iPS cells

Zygotes

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CRISPR/Cas9 Genome engineering Applications in regenerative medicine

http://www.youtube.com/watch?v=0dRT7slyGhs

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CRISPR/Cas9 Genome engineering Repair of Cystic Fibrosis Gene CFTR

(cystic fibrosis transmembrane conductor receptor)

Schwank et al., Cell Stem Cell 2013

Forskolin -> CFTR -> expansion

In vitro assay in intestinal organoids:

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Stem Cell and Gene Therapy

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ANAT3231: lectures overview

Dr Annemiek Beverdam – School of Medical Sciences, UNSW Wallace Wurth Building Room 234 – [email protected]

Stem Cell Technology

Regenerative Medicine Stem Cell Sources

Future of Regenerative Medicine Knock-out Technology

CRISPR/CAS9 Genome Editing